Joint Annual
Meeting ISMRM-ESMRMB 2014
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10-16 May 2014
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Milan, Italy |
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TRADITIONAL
POSTER SESSION ○ CANCER |
Breast Cancer: Clinical
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
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1029. |
Breast PET/MRI correlations
between SUVmax, ADCmin, tumor markers and systemic disease
Amy Melsaether1, Akshat C. Pujara2,
Eric Sigmund2, Alana Amarosa2,
Freya Schnabel2, Deirdre Kiely2,
Sungheon Kim2, and Linda Moy2
1NYU, New York, New York, United States, 2NYU,
New York, United States
In this preliminary study, we address whether the PET
and DWI data (SUV max and ADC min) acquired during a
breast PET/MRI correlate with each other and with breast
cancer tumor markers and with systemic disease.
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1030. |
Assessment of High Spatial
Resolution 3D T2W Fat Nulled Images: a Comparison with 2D
T2W Fat Sat Images
Martin D Pickles1, Daniel Litwiller2,
and Lindsay W Turnbull1
1Centre for Magnetic Resonance
Investigations, HYMS at University of Hull, Hull, East
Yorkshire, United Kingdom, 2Global
MR Applications and Workflow, GE Healthcare, Rochester,
MN, United States
Further improvements in the specificity of MR breast are
required. Recently, a 3D FSE T2W modified 3-point DIXON
technique (CUBE-IDEAL) became available. The purpose of
this work is to evaluate CUBE-IDEAL and compare against
traditional 2D T2W FSE fat saturated images. Sixty-nine
patients were imaged on a 3.0T scanner. The results of
this assessment suggest a similar level of performance
overall. However, a number of key points should be
underscored. Firstly, CUBE-IDEAL did outperform FSE at
fat nulling. Secondly, CUBE-IDEAL can be reformatted
into any plane. Thirdly, CUBE-IDEAL presents a time
saving over the traditional FSE sequence.
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1031. |
DWI of Breast at 3T:
Effects of Fibroglandular Tissue Composition and Background
Parenchymal Enhancement in Patients with Malignant and
Benign Lesions
Soledad Milans1, Sujata Patil2,
Elizabeth Morris2, and Sunitha Thakur1
1Memorial Sloan-Kettering Cancer Center, New
York, NY, United States, 2Memorial
Sloan-Kettering Cancer Center, NY, United States
The amount of fibroglandular tissue (FGT) density and
the level of background parenchymal enhancement (BPE)
are MRI features of normal breast. Studies showed
increased BPE to be strongly predictive of breast cancer
odds as with increased FGT. We propose to evaluate the
effect of FGT density and BPE on ADC values in patients
with malignant and benign findings at 3.0T. FGT-ADC
values were significantly higher in patients with
malignant lesions with higher density compared to lower
density (p=0.0073). In patients with benign lesions,
difference is smaller between both groups (p=0.015). No
significant difference was observed in FGT-ADC values
with BPE.
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1032. |
Diffusion MRI and in-vivo
proton MR Spectroscopy Study of the Differentiation of
Malignant Breast Tissue of Breast Cancer Patients and the
Normal Breast tissue of Healthy Lactating Women Volunteers
Naranamangalam R Jagannathan1, Khushbu
Agarwal1, Rani G Sah1, Uma Sharma1,
Rajinder Parshad2, and Vurthaluru Seenu2
1Department of NMR & MRI Facility, All India
Institute of Medical Sciences, New Delhi, Delhi, India, 2Department
of Surgical Disciplines, All India Institute of Medical
Sciences, New Delhi, Delhi, India
Diffusion weighted imaging and in-vivo proton MRS in
lactating women volunteers (n=16) and in patients with
breast cancer (n=13) showed total choline peak in 16/16
malignant cases and in 11/13 lactating women volunteers.
Further, 11/13 of lactating women showed a lactose peak
at 3.8 ppm. tCho concentration was similar in both
groups while higher ADC was observed in lactating women.
Our study demonstrated that higher ADC value together
with the presence of a lactose peak may aid in the
differentiation of changes that occur in the breast
tissues due to normal physiological conditions as
compared with malignant transformations.
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1033. |
A comparison of Short and
Standard Exam Time Breast MR Studies
Martin D Pickles1, Lindsay W Turnbull1,
Peter Gibbs1, and Martine Dujardin1
1Centre for Magnetic Resonance
Investigations, HYMS at University of Hull, Hull, East
Yorkshire, United Kingdom
We believe that a short breast MR examination contains
the necessary information to allow an accurate
diagnosis. The purpose of this study is to determine the
technical feasibility of a short examination and to
obtain preliminary comparative data against the standard
examination. Nineteen participants were imaged on a 3.0T
scanner twice (standard and short). Results suggest that
the short breast MR examination is not only feasible but
has good agreement with the standard examination. This
study has demonstrated that high spatial and temporal
resolution data can be acquire in only 12minutes with
similar results to much longer MR examinations.
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1034. |
Correlation of electric
conductivity with prognostic factors in invasive breast
cancer
Soo-Yeon Kim1, Jaewook Shin2,
Dong-Hyun Kim2, Min-Jung Kim1, and
Eun-Kyung Kim1
1Radiology, Severance Hospital, Yonsei
University College of Medicine, Seoul, Seodaemun-gu,
Korea, 2Electronic
and Electronic Engineering, Yonsei University, Seoul,
Seodaemun-gu, Korea
The electric conductivity has shown its potential to
differentiate benign and malignant breast tissue. We
investigate the correlation between the electric
conductivity with known prognostic factors of invasive
breast cancer using the electric properties tomography
reconstruction algorithm and multi-receive coil combined
technique. Breast cancers with the established poor
prognostic factors (axillary lymph node metastasis,
lymphovascular invasion and high histologic grade)
showed higher conductivity value than those without. Our
results show the possibility that the electric
conductivity can be differentiated according to the
known prognostic markers in invasive breast cancers.
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1035. |
Breast Cancer Assessment
Based on Perfusion Dependence in Diffusion Weighted Imaging
using Different Monoexponential Fitting Schemes
Jose Ramon Teruel1,2, Agnes Østlie3,
Hans Erikssønn Fjøsne4,5, Tone Frost Bathen1,
and Pål Erik Goa2,6
1Department of Circulation and Medical
Imaging, NTNU, Trondheim, Norway, 2St.
Olavs University Hospital, Trondheim, Norway, 3Department
of Radiology, St. Olavs University Hospital, Trondheim,
Norway, 4Department
of Surgery, St. Olavs University Hospital, Trondheim,
Norway, 5Institute
of Cancer Research and Molecular Medicine, NTNU,
Trondheim, Norway, 6Department
of Physics, NTNU, Trondheim, Norway
In this study, a simplified approach to obtain perfusion
influence from diffusion weighted imaging (DWI)
measurements for breast cancer assessment is proposed.
Our results present how the relative perfusion effect
derived from different monoexponential fitting schemes
of DWI measurements can be obtained. Furthermore, this
simplified approach offers a potential for breast cancer
differentiation by means of the derived biomarker.
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1036. |
Breast dynamic MR features
including texture analysis associated with pathologic
prognostic factors in triple negative breast cancers.
Bo La Yun1, Sun Mi Kim1, Mijung
Jang1, Hye Shin Ahn1, Kyung Eun
Cho1, Bohyoung Kim1, Hochul Kang2,
and Ji Young Kim1
1radiology, Seoul national Univ. Bundang
Hosp., Seoungnam-si, Kyongki-do, Korea, 2Seoul
national Univ, Seoul, Korea
Triple negative breast cancers are heterogeneous disease
and poor prognosis. We were investigated early and
delayed enhancement pattern and texture feature on
breast dynamic MR image. In this study, We found that
early and delayed enhancement pattern (rapid and plateu)
and texture features (high entropy and low homogniety)
in breast dynamic MR were associated with traditional
pathologic poor prognosis factors in triple negative
breast tumor. These image features could predict
preoperative breast cancer aggressiveness.
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1037. |
Detection of altered
adipose tissue composition in breast cancer patients using
MR spectroscopy
Palamadai N Venkatasubramanian1, George
Iordanescu1, Matthew M Smith1,
Jennifer L Gnerlich2, Katherine Yao3,
and Alice M Wyrwicz1
1Radiology, NorthShore University
HealthSystem, Evanston, IL, United States, 2Surgery,
The University of Chicago Medical Center, Chicago, IL,
United States, 3Surgery,
NorthShore University HealthSystem, Evanston, IL, United
States
Using ex vivo MR spectroscopy we found alterations in
the fatty acid composition of peritumoral adipose tissue
from breast cancer patients, relative to adipose tissue
from a distal location within the same breast. MR-measured
compositions of breast adipose tissues could predict
known pathological criteria for invasive breast cancers.
Our results suggest that in vivo MRS may have potential
for developing a noninvasive biomarker for invasive
breast cancers.
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1038. |
Lipid Deregulation in Women
Carrying the BRCA Mutations: Non invasive evaluation by
two-dimensional Spectroscopy
Saadallah Ramadan1, Jameen Arm2,
Gorane Santamaria3, Judith Silcock4,
Jessica Buck5, Michelle Roy6, Kin
Men Leong7, Peter Lau7, David
Clark4, Peter Malycha6, and
Carolyn Mountford6
1School of Health Sciences, University of
Newcastle, Callaghan, NSW, Australia, 2Hunter
New England Health, The Mater Hospital, Callaghan, NSW,
Australia, 3Department
of Radiology, Hospital Clinic de Barcelona, Villarroel,
Spain, 4The
Breast & Endocrine Centre, NSW, Australia, 5School
of Health Sciences, University of Newcastle, NSW,
Australia,6School of Health Sciences, Centre
for MR in Health, NSW, Australia, 7Calvary
Mater Hospital, NSW, Australia
BRCA1 and BRCA2 genes belong to the tumor suppressor
family and patients with these genes are at increased
risk of developping breast cancer. In this study, we
apply in vivo two-dimensional 2D localized correlation
spectroscopy (L-COSY) to look for a premalignant state
in the breast tissues of apparently healthy women
carrying the BRCA gene mutations and others with a
family history. We propose the hypothesis that those
with the BRCA gene mutations would have altered
chemistry reflective of a preinvasive state.
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1039. |
Errors Associated with
Followup Measurments of ADC in Assessing Response to
Neoadjuvant Chemotherapy
Shelley Waugh1, Lukasz Priba1, and
Sarah Vinnicombe2
1Medical Physics, Ninewells Hospital, Dundee,
Angus, United Kingdom, 2Division
of Cancer Research, University of Dundee, Dundee, United
Kingdom
This study considers the use of apparent diffusion
coefficient (ADC) measures as an indicator of early
response to neoadjuvant chemotherapy. As ADC changes are
utilised in clinical practice, this investigation
considers the multiple factors that may influence these
measurements and could influence classification of
response according to RECIST criteria. Scanner
stability, scan-scan repeatability and intra-observer
repeatability are measured with reference to the order
of magnitude of ADC changes likely to be encountered in
clinical patients who respond, partially respond and
have stable disease.
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1040. |
Acoustic radiation contrast
in magnetic resonance to visualize viscoelastic properties
in human breast - preparation of clinical trial
Judith Wild1, Anna-Lisa Kofahl1,
Deniz Ulucay1, Sebastian Theilenberg1,
Carsten Urbach1, Jürgen Finsterbusch2,
Kerstin Rhiem3, Peter Trautner4,
and Karl Maier1
1University of Bonn, Bonn, Germany, 2University
Medical Center Hamburg, Hamburg, Germany, 3University
Medical Center Cologne, Cologne, Germany, 4Life
& Brain GmbH, Bonn, Germany
The early detection of breast cancer has severely
improved during the past 20 years, but there is still
room for improvement like a better clarification of
indications without using ionizing radiation. The
evaluation of biopsy data showed that about 80% of women
diagnosed with cancer after the different types of
imaging do not have cancer. We target on improving this
high percentage by improving the specificity by
measuring the elasticity of lesions. Measurements on 10
volunteers with well known lesions provide an important
step towards seeing if ARC-MR is capable to improve the
specificity of standard breast cancer diagnostic.
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1041. |
Comparison of steady-state
and spin-echo DWI based on morphological assessment of
breast lesions
Kristin L Granlund1,2, Debra Ikeda1,
Jafi Lipson1, Jennifer Kao1, Jung
Min Chang3, Brian Hargreaves1, and
Bruce Daniel1
1Radiology, Stanford University, Stanford,
CA, United States, 2Electrical
Engineering, Stanford University, Stanford, CA, United
States, 3Radiology,
Seoul National University Hospital, Seoulq, Korea
The DESS sequence has been used to acquire
diffusion-weighted images, and this study evaluates DESS
images relative to EPI DWI images. Four radiologists
were surveyed about the image quality and BI-RADS scores
of images containing pathology-proven breast lesions.
The DESS sequence acquired sharper diffusion-weighted
breast images than EPI (p<0.001). ROC curves were
calculated from the BI-RADS scores, and the DESS
sequence had a larger AUC (0.74 for DESS, 0.68 for EPI)
and a tighter confidence interval. Better image quality
facilitates morphological assessment of lesion
malignancy.
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1042. |
Comparison of the value of
DWI based on monoexponential and stretched exponential model
in differential diagnosis between benign and malignant
lesions of breast
Jie He1, Yan Zhang1, Jingliang
Cheng1, Ying Hu1, Anfei Wang1,
Dandan Zheng2, and Xiaoyan Wang1
1Department of MRI, the First Affiliated
Hospital of Zhengzhou University, Zhengzhou, HeNan,
China, 2GE
healthcare, Beijing, China
MRI has been widely used in the diagnosis of breast
disease. However, the calculation of apparent diffusion
coefficient by simple monoexponential relationship
between MRI signal and b value does not fully account
for tissue behavior. Intravoxel incoherent motion (IVIM)
method allows quantitative parameters that reflect
tissue micro capillary perfusion and tissue diffusivity.
In this study, the stretched-exponential model was used
to generate ¦Á and distributed diffusion coefficient (DDC)
maps. The ¦Á values and DDCs were compared with
traditional monoexponential ADC in the differential
diagnosis of breast benign and malignant lesions.
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TRADITIONAL
POSTER SESSION ○ CANCER |
Breast Cancer: Technical
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
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1043. |
Correlation of percent
breast density with background parenchymal enhancement
measured in MRI
Jeon-Hor Chen1,2, Yifan Li1, Hon
Yu1, Shadfar Bahri1, Rita S Mehta3,
and Min-Ying Su1
1Center for Functional Onco-Imaging,
University of California, Irvine, California, United
States, 2Department
of Radiology, Eda Hospital and I-Shou University,
Kaohsiung, Taiwan, 3Department
of Medicine, University of California, Irvine,
California, United States
In this study we aimed to correlate percent breast
density (PD) and background parenchymal enhancement (BPE)
in the contralateral normal breast (CNB) of patients
diagnosed with breast cancer. Breast MR images of the
CNB of 117 patients were studied. The quantification of
the fibroglandular tissue volume (FV) was based on a
computer-assisted algorithm. The mean BPE and the hot
spot enhancement were correlated with age, and also with
FV and PD. Our study showed that BPE, measured by the
averaged enhancement of the whole FV or by hot spot, did
not correlate well with quantitative measurement of PD
and FV.
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1044. |
Impact of positional
difference on the measurement of breast density in MRI
Jeon-Hor Chen1,2, Siwa Chan3,
Yi-Ting Tang4, Angela T. Cheriyan1,
Nikita Rakesh Shah1, and Min-Ying Su1
1Center for Functional Onco-Imaging,
University of California, Irvine, California, United
States, 2Department
of Radiology, Eda Hospital and I-Shou University,
Kaohsiung, Taiwan, 3Department
of Radiology, Taichung Veterans General Hospital,
Taichung, Taiwan, 4Department
of Medical Imaging, China Medical University, Taichung,
Taiwan
We conducted a study to investigate the consistency of
percent breast density measured in MRI in four different
positions and imaging resolution. The breast and
fibroglandular tissue segmentation was based on an
established novel method. Results of FV and PD
measurement show small variations, with an averaged CV
of <9%, among the four MR studies. Remarkable
measurement variation did occur in some subjects in
hands-down position, compared to hands-up position. The
results from our MR consistency study indicate that MR
imaging data from multi-centers, regardless of patients’
positions (hand-up or hands-down), can be combined for
analysis.
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1045. |
VOLUMETRIC BREAST DENSITY
QUANTIFICATION FROM 2D MAMOGRAPHIES COMPARED WITH BREAST MRI
Camila Munoz1, Dravna Razmilic2,
Maria E. Navarro2, Paula Espinoza2,
Cristian Tejos1, Pablo Irarrazaval1,
Sergio Uribe1, and Marcelo E. Andia1,2
1Biomedical Imaging Center, Pontificia
Universidad Catolica de Chile, Santiago, Region
Metropolitana, Chile, 2Radiology
Department, School of Medicine, Pontificia Universidad
Catolica de Chile, Santiago, Region Metropolitana, Chile
Breast density is a major risk factor of breast cancer,
and is usually assessed visually from mammograms. This
has two main disadvantages: there is not a standard
measure of breast density, as the breast is classsified
in qualitative categories, and this assessment does not
consider that mammography is a 2D projection of the
breast volume. We developed a method to quantify
volumetric breast density from mammograms and a
semi-automatic method that quantifies this measure in 3D
breast MRI. Thus, it is possible to obtain an equivalent
quantitative measure of breast density between both
imaging techniques, solving the issues mentioned above.
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1046. |
A novel and affordable DCE-MRI
phantom: Prospective assessment of DCE-MRI breast protocols
Araminta E. W. Ledger1, Marco Borri1,
Hector Sanchez Casas1, Craig Cummings1,
Maria A. Schmidt1, and Martin O. Leach1
1CR-UK and EPSRC Cancer Imaging Centre, The
Institute of Cancer Research and Royal Marsden NHS
Foundation Trust, Sutton, Surrey, United Kingdom
DCE-MRI is an established component of breast screening
protocols, and uses the empirical classification of
contrast agent (CA) enhancement curves to aid diagnosis.
However, CA enhancement curves resulting from varying
parameter selections are difficult to assess
prospectively. This abstract uses a novel and affordable
DCE-MRI phantom to assess the effect of common sequence
alterations (CA injection timing and k-space sampling
scheme) on the CA enhancement curves obtained from two
clinical DCE-MRI sequences. Both CA injection timing and
k-space sampling pattern resulted in measurable curve
differences - sequence comparison with this phantom can
therefore help to establish robust DCE-MRI breast
protocols.
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1047. |
Universal Breast Phantom
for Quantitative MRI
Kathryn E Keenan1, Sheye O Aliu2,
Lisa J Wilmes2, David C Newitt2,
Elizabeth Horneber3, Karl F Stupic1,
Michael A Boss1, Michael G Snow4,
William Hollander4, Stephen E Russek1,
and Nola M Hylton2
1National Institute of Standards and
Technology, Boulder, CO, United States, 2University
of California San Francisco, San Francisco, CA, United
States, 3University
of Colorado, Boulder, CO, United States, 4High
Precision Devices, Boulder, CO, United States
A novel breast phantom was created for the breast
imaging community for implementation of quality control
measures. The phantom contains well-distributed fat and
fibroglandular T1 relaxation mimics and diffusion
mimics. In addition, the phantom has a flexible outer
shell so that it is compatible with several coil
designs. In initial testing, the phantom fit in several
coil designs, enabled fat-suppression tests, and allowed
assessment of diffusion artifacts. Please visit our
website for additional information: http://collaborate.nist.gov/mriphantoms/bin/view/MriPhantoms/BreastPhantom.
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1048. |
A Simulation Study of the
Flexible TWIST View Sharing Impact on the Breast DCE MRI
Yuan Le1, Marcel Dominik Nickel2,
Randall Kroeker2, Christian Geppert2,
Brian Dale2, Hal D. Kipfer3, and
Chen Lin1
1Radiology and Imaging Science, Indiana
University School of Medicine, Indianapolis, Indiana,
United States, 2Siemens
Healthcare, North Carolina, United States, 3Radiology
and Imaging Science, Indiana University School of
Medicine, Indiana, Indiana, United States
The acquisition of breast DCE-MRI using a flexible TWIST
view sharing technique was simulated. A digital
‘phantom’ was generated with three 5mm uniform spherical
lesions of ‘persistent’, ‘plateau’ and ‘wash-out’ type
of contrast uptake, and one 10 mm complex tumor with a
mixture of all three types of enhancements. Our results
show that with the typical spatial resolution in
clinical breast DCE-MRI, TWIST view sharing parameters
of pA=20% and pB=20% provides the lowest overall RMS
error for all time points, while pA=50% and pB=50%
produces image with minimum error at the peak contrast
uptake.
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1049. |
Clinical Feasibility of
CAIPIRINHA-Dixon-TWIST (CDT)-Volume-Interpolated Breath-Hold
Examination (VIBE) for Breast DCE-MRI
Wen Hao1, Bin Zhao1, Guangbin Wang1,
Hui Liu2, and Cuiyan Wang1
1Magnetic resonance imaging, Shandong medical
imaging research institution, Shandong University,
Jinan, ShanDong, China, 2MR
Collaboration NEA, Siemens Healthcare, Shanghai, China
This abstract is about assessment performed to
investigate the clinical feasibility of CDT-VIBE for
quantitative breast DCE-MRI. In conclusion, we believe
that CDT-VIBE can be used in breast DCE-MRI for
detecting and depicting lesions because of its high
spatial resolution and nearly equal image quality to
conventional VIBE image. Therefore, it is clinically
feasible to replace standard 60-90 second conventional
GRE sequence by CDT-VIBE sequence for quantitative
breast DCE-MRI with the acquisition schemes employed in
this study.
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1050. |
Self-Organizing Map Kinetic
Features as Prognostic Markers for Classifying Gene
Expression Risk for Breast Cancer Recurrence
Majid Mahrooghy1, Ahmed B. Ashraf1,
Dania Daye1, Carolyn Mies2, Mark
Rosen1, Michael Feldman2, and
Despina Kontos1
1Department of Radiology, University of
Pennsylvania, Philadelphia, PA, United States, 2Department
of Pathology and Laboratory Medicine, University of
Pennsylvania, Philadelphia, PA, United States
We developed DCE-MRI kinetic heterogeneity features
using self-organizing map (SOM) neural networks. We use
SOM to cluster tumor pixels based on kinetics and
extract features including variance and entropy of
cluster size, variance of cluster kinetic features, mean
and variance of weighted cluster kinetics, and the
kinetic features of the cluster having maximum peak
enhancement. We evaluated these features for classifying
tumor recurrence risk as determined by a validated gene
expression assay, and compared their performance to
current standard kinetics. Our features have ROC AUC=0.80
for classifying tumors at low- versus high- risk of
recurrence, outperforming standard kinetics with AUC=0.65.
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1051. |
Non-Rigid-Registration of
Breast Dynamic Contrast-Enhanced MRI Data: Comparison and
Evaluation of B-splines and Symmetric Diffeomorphic
Normalization based Methods
Venkata Veerendranadh Chebrolu1, Dattesh D
Shanbhag1, Aurelie Le Deley2,
Sheshadri Thiruvenkadam1, Uday Patil1,3,
Patrice Hervo2, Sandeep N Gupta4,
and Rakesh Mullick5
1Medical Image Analysis Lab, GE Global
Research, Bangalore, Karnataka, India, 2GE
Healthcare, Buc, France, 3Manipal
Health Enterprises Pvt. Ltd., Bangalore, Karnataka,
India,4Biomedical Image Processing Lab, GE
Global Research, Niskayuna, NY, United States, 5Diagnostics
and Biomedical Technologies, GE Global Research,
Bangalore, Karnataka, India
DCE-MRI is increasingly being used in diagnosis and
screening of breast tumors. Careful study of intensity
changes over time between the pre-contrast and
post-contrast images is critical to tumor biometry.
Rigid and non-rigid motion may be caused by factors such
as voluntary patient motion, cardiac pulsation, and
breathing during image acquisition. In this work we
compare and evaluate b-splines and symmetric
diffeomorphic normalization based non-rigid registration
(NRR) algorithms for their effectiveness in motion
correction for breast DCE-MRI. B-splines based NRR
approaches provided consistent time performance. Better
NRR accuracy was achieved with diffeomorphic
normalization based motion correction methods.
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1052. |
Multi Slice-Group
Slice-Accelerated Breast Diffusion MR Imaging on 3T
Sinyeob Ahn1, Himanshu Bhat1,
Dorota Wisner2, Kawin Setsompop3,
Thomas Benner4, Stephen Cauley3,
Borjan Gagoski5, Bonnie Joe2,
Gerhard Laub1, and Vibhas Deshpande1
1Siemens Healthcare, San Francisco, CA,
United States, 2Radiology
and Biomedical Engineering, UCSF, CA, United States, 3Radiology,
MGH, MA, United States, 4Siemens
Healthcare, Erlangen, Germany, 5Children's
Hospital, Boston, MA, United States
Brest diffusion MRI has been typically performed in an
axial slice orientation with large FOV which tends to
show ghosting artifacts from significant B0 field
inhomogeneity. Sagittal slice orientation is limited due
to long scan time. In this paper, we propose a multiple
slice group slice-accelerated sequence for sagittal
bilateral breast diffusion imaging. One slice on each
slice group out of two was acquired and compared to the
standard technique. The proposed method provided nearly
identical image quality with almost half the scan time
as compared to the standard bilateral diffusion imaging,
suggesting a viable tool for breast lesion
characterization within reasonable scan time.
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1053. |
Factors Affecting ADC
Measures in Breast Cancer Patients
Shelley Waugh1, Lukasz Priba1, and
Sarah Vinnicombe2
1Medical Physics, Ninewells Hospital, Dundee,
Angus, United Kingdom, 2Division
of Cancer Research, University of Dundee, Dundee, United
Kingdom
The aim of this study was to identify the contribution
of various factors that may have an impact on accuracy
of measurements of apparent diffusion coefficients (ADC)
in breast MRI. We have considered the effect of
long-term scanner stability, positional dependence
within the coil, scan-scan repeatability and the effect
of single and multiple observers on final measurements
of whole tumour and lowest ADC values within tumours. We
conclude that scan-scan repeatability and scanner
stability have minimal effect on measured ADC values and
the biggest influence on measured ADC values is
inter-observer repeatability.
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1054. |
DW-MP-SWIFT for High
Spatial Resolution Diffusion Weighted Breast MRI
Curtis A. Corum1, Djaudat Idiyatullin1,
Diane Hutter1, Lenore I. Everson1,
Lynn E. Eberly2, Michael T. Nelson3,
and Michael Garwood1
1CMRR, Radiology, Medical School, University
of Minnesota, Minneapolis, Minnesota, United States, 2Biostatistics,
School of Public Health, University of Minnesota,
Minneapolis, Minnesota, United States, 3Breast
Center, Radiology, Medical School, University of
Minnesota, Minneapolis, Minnesota, United States
This work describes a diffusion-weighted magnetization
prepared SWIFT (SWeep Imaging with Fourier
Transformation) sequence utilizing adiabatic RF pulses
for diffusion weighting with additional fat suppression.
The SWIFT sequence is used as excitation and high
resolution readout of the prepared diffusion-weighted
and fat-suppressed magnetization. The proposed method,
DW-MP-SWIFT, is more robust to motion and eddy currents
compared to typical diffusion-weighted sequences, while
providing high spatial resolution. We report results of
DW-MP-SWIFT for phantom and breast imaging of normal
human subjects.
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1055. |
High Spatial Resolution DTI
Sequence for Characterizing Breast Tumor Early Treatment
Response: Comparison to Standard DTI Sequence
Lisa Wilmes1, Wei Ching Lo2, David
C Newitt2, Suchandrima Banerjee3,
Evelyn Proctor2, Emine Saritas4,
Ajit Shankaranarayanan3, and Nola M Hylton2
1University of California San Francisco, San
Francisco, CA, United States, 2University
of California San Francisco, CA, United States, 3Applied
Science Laboratory GE Healthcare, CA, United States, 4University
of California Berkeley, CA, United States
A high-resolution reduced field of view diffusion tensor
weighted imaging sequence (HR-DTI), voxel size 4.8 mm3,
was optimized for breast imaging and compared to a
standard FOV DTI sequence (STD-DTI), voxel size 29.3
mm3, for evaluating tumor response to treatment in seven
breast cancer patients undergoing neoadjuvant
chemotherapy. Significant differences were found between
the tumor fractional anisotropy (FA) measured by HR-DTI
and the STD-DTI prior to and early in treatment. Of the
DTI parameters evaluated, HR-DTI FA correlated most
strongly with tumor volume change post treatment. This
preliminary study suggest that HR-DTI may be sensitive
to treatment-induced changes in tumors.
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1056. |
Longitudinal variation of
fibroglandular tissue and background parenchymal enhancement
on breast MRI in high-risk women: a quantitative assessment
Shandong Wu1, Wendie A. Berg2,
Margarita L. Zuley2, Jules Sumkin2,
Rachel C. Jankowitz3, and David Gur4
1Radiology, University of Pittsburgh,
Pittsburgh, PA, United States, 2Radiology,
University of Pittsburgh Medical Center Magee-Womens
Hospital, PA, United States, 3Oncology,
University of Pittsburgh Medical Center Magee-Womens
Hospital, PA, United States, 4Radiology,
University of Pittsburgh, PA, United States
The purpose of this study is to perform quantitative
assessment on the longitudinal variation of
fibroglandular tissue (FGT) and background parenchymal
enhancement (BPE) in sequential breast MRI scans for a
cohort of high-risk women of developing breast cancer
who did not undergo any specific risk-reduction
intervention. We retrospectively analyzed 71 high-risk
women each with two longitudinal cancer-free MRI scans
using a fully automated computerized method. The
preliminary results demonstrate the temporal variability
of FGT and BPE, which may be useful as a reference
measure when investigating these parameters as risk
predictors and possibly as indicators of
intervention-response in high-risk women.
|
1057. |
Type Discrimination of
Calcifications using High-pass Filtered Phase Images of
Multiple Fast Field Echo Sequence
Katsuhiro Kida1, Sachiko Goto2,
Tsutomu Kajitani1, and Yoshiharu Azuma2
1Department of Radiology, Japanese Red Cross
Okayama Hospital, Okayama-shi, Okayama, Japan, 2Faculty
of Health Sciences, Graduate School of Health Sciences,
Okayama University, Okayama-shi, Okayama, Japan
In this study, we discriminated the calcium oxalate and
calcium phosphate in breast disease. A cup shaped gel
phantom containing two types kidney stones was employed
to simulate calcification in the breast. The phase
values of five phase images with different echo times
were measured, those were obtained by a 3D m-FFE
sequence to shorten examination time. We conclude that
the calcium oxalate and phosphate are distinguishable
with the slope of linear approximation of calcifications
on high-pass filtered phase images. We believe that this
method is useful for the discrimination between benign
and malignant breast disease.
|
1058. |
Using MRI to characterize
lymphatic structure and function without exogenous contrast
agents
Paula Donahue1, Swati Rane2, Seth
Smith2, and Manus Donahue2
1Physical Medicine and Rehabilitation, Dayani
Center for Health and Wellness, Vanderbilt University
School of Medicine, Nashville, TN, United States, 2Radiology,
Vanderbilt University School of Medicine, TN, United
States
The overall objective of this work is to translate
noninvasive imaging techniques for measuring brain
structure and function to the lymphatic system to
characterize axillary lymphatic vessel structure and
interstitial protein accumulation in patients with
breast cancer-related lymphedema (BCRL). To achieve
this, a multi-faceted, noninvasive 3T MRI protocol for
characterizing lymph node volume (DWIBS MRI), lymph
vessel diameter (3D TSE), lymph flow velocity (spin
labeling MRI), and interstitial protein accumulation
(APT CEST MRI) are optimized and applied in healthy
volunteers (n=10) and patients with BCRL (n=4).
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|
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TRADITIONAL
POSTER SESSION ○ CANCER |
Prostate Cancer
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
|
|
1059. |
Metabolomic Imaging for
Human Prostate Cancer Detection using MR Spectroscopy at 7-T
Romy Langhammer1,2, Leo L. Cheng1,
Johannes Nowak3, Shulin Wu1, W.
Scott McDougal1, Chin-Lee Wu1, and
Eva M. Ratai1
1Massachusetts General Hospital, Harvard
Medical School, Boston, Massachusetts, United States, 2Institute
of Radiolgy, Department for Neuroradiology, University
Hospital Wuerzburg, Wuerzburg, Bavaria, Germany, 3Institute
of Radiology, Department for Neuroradiology, University
Hospital Wuerzburg, Wuerzburg, Bavaria, Germany
The project aims to develop a non-invasive diagnostic
test for prostate cancer. Metabolomic imaging maps of
thirty whole prostates were created and analyzed, using
magnetic resonance spectroscopy (MRS) at 7T. To test the
functionality and reliability of this system, the
outcome has been compared with the histopathology
findings. In 61% of the samples, MRS detected cancer
lesions in the same locations as were identified in the
histopathology analysis; the histological regions that
were not detected had significantly lower tumor volumes.
Furthermore, a "Malignancy Index" can significantly
differentiate between cancerous and benign MRS
suspicious regions.
|
1060.
|
Fast 1H-MRSI
of the prostate with GOIA-sLASER localization and spiral
acquisition
Isabell K. Steinseifer1, Bart Philips1,
Borjan Gagoski2, Marnix C. Maas1,
Elisabeth Weiland3, Tom W.J. Scheenen1,
and Arend Heerschap1
1Radiology, Radboud University Medical
Center, Nijmegen, Netherlands, 2Fetal-Neonatal
Neuroimaging & Developmental Science Center, Boston
Children's Hospital, Harvard Medical School, Boston, MA,
United States, 3MR
Applications Development, Siemens AG, Healthcare Sector,
Erlangen, Germany
Fast 1H
MRSI of the prostate was achieved with a semi-LASER
sequence with GOIA-WURST(16,4) refocusing pulses and
spiral k-space sampling. The application of these low RF
power demanding adiabatic pulses reduces the specific
absorption rate so that an endorectal coil can be used
to receive signal. Together with a relative short echo
time of 90ms, a high SNR can be obtained. This can be
translated in a much lower acquisition time, which can
be realized because of the flexibility of spiral k-space
sampling. The new sequence facilitates routine
acquisition of metabolic data for clinical purposes.
|
1061. |
Carbon Ion Radiation
Therapy for Patients with Localized Prostate Cancer:
Maya B Wolf1, Timur H Kuru2,
Gregor Habl3, and Matthias C Roethke1
1Radiology, DKFZ, Heidelberg,
Baden-Württemberg, Germany, 2Urology,
University Hospital Heidelberg, Heidelberg,
Baden-Württemberg, Germany, 3Radiation
Oncology, University Hospital Heidelberg, Heidelberg,
Baden-Württemberg, Germany
Purpose was to assess T2- and diffusion-weighted imaging
(DWI) after carbon ion therapy (CIT) of prostate cancer
(PCa) for treatment monitoring. Multiparametric MRI
including T2 and DWI at 3T were acquired prior to and
following CIT in patients with histologically confirmed
PCa. Statistical analysis of region of interest data
showed T2w signal loss at the 6 months interval and
immediate, as well as, continuous apparent diffusion
coefficient (ADC) increase after treatment in PCa areas.
PSA was inversely correlated with ADC values. The
results suggest that ADC could serve as an imaging
biomarker for assessing therapeutic response of PCa to
CIT.
|
1062. |
Quantitative evaluation of
diffusion weighted imaging techniques for radiotherapy of
prostate cancer
Gary Liney1,2, Thahabah Mohammed Al Harthi3,
Ewa Juresic4, Lynette Cassapi4,
Lois Holloway4, Mark Sidhom4,
David Manton5, and Peter Gibbs6
1Medical Physics, Ingham Institute for
Applied Medical Research, Sydney, NSW, Australia, 2Physics,
University of Wollongong, Sydney, NSW, Australia, 3Physics,
University of Sydney, NSW, Australia, 4Cancer
Therapy Centre, Liverpool Hospital, NSW, Australia, 5Radiation
Physics, East Riding, United Kingdom, 6University
of Hull, East Riding, United Kingdom
The measurement of apparent diffusion coefficient (ADC)
from diffusion weighted imaging (DWI) has been linked to
tumour response following radiotherapy in prostate
cancer. For it to be used to monitor and adapt plans
during a course of treatment DWI needs to be produce
reliable measurements and distortion free images. This
work compares three DWI techniques in phantoms and
prostate volunteers in order to assess their suitability
for use as a robust clinical tool.
|
1063. |
Multiparametric 3T prostate
MRI in patients with elevated PSA and no previous biopsy
Ivan Jambor1, Esa Kähkönen2, Pekka
Taimen3, Harri Merisaari4, Jani
Saunavaara5, Kalle Alanen6,
Branislav Obsitnik7, Heikki Minn4,
Viera Lehotska8, and Hannu Aronen1
1Departement of Diagnostic Radiology,
University of Turku, Turku, Finland, 2Department
of Surgery, Turku University Hospital, Turku, Finland, 3Department
of Pathology, University of Turku, Turku, Finland, 4Turku
PET centre, University of Turku, Turku, Finland, 5Medical
Imaging Centre of Southwest Finland, Turku University
Hospital, Turku, Finland, 6Department
of Pathology, Turku University Hospital, Turku, Finland, 7Department
of Urology, St. Elisabeth Oncology Institute,
Bratislava, Slovakia,8Department of
Radiology, St. Elisabeth Oncology Institute, Bratislava,
Finland
Fifty-five patients with elevated PSA (>4 ng/ml), no
previous biopsy and low risk of prostate cancer (PCa)
underwent mpMRI at 2 institutions (41 at institution A
and 14 patients at institution B), consisting of
anatomical T2-weighted imaging (T2wi), diffusion
weighted imaging (DWI), proton magnetic resonance
spectroscopy and dynamic contrast enhanced MRI, using
surface array coils followed by MRI targeted TRUS-guided
biopsy in addition to 12 core systematic biopsy. The use
of T2wi+DWI was shown to be an accurate tool for initial
decision management and targeting biopsy in patients
with elevated PSA.
|
1064. |
Comparative Study of Four
Widely used Classifiers for Prostate Cancer Detection with
Multi-parametric MRI
Chengyan Wang1, Shuangjuan Cheng2,
Juan Hu2, He Wang2, Xuedong Yang2,
Jue Zhang1,3, Xiaoying Wang1,2,
and Jing Fang1,3
1Academy for Advanced Interdisciplinary
Studies, Peking University, Beijing, Beijing, China, 2Department
of Radiology, Peking University First Hospital, Beijing,
Beijing, China,3College of Enigneering,
Peking University, Beijing, Beijing, China
Prostate cancer (PCa) is the second most frequently
diagnosed cancer and the sixth leading cause of cancer
death among men worldwide [1]. Several studies [2-4]
have proven that the diagnostic accuracy of PCa
detection can be significantly improved by combining
different MR sequences, and several computer-aided
diagnosis (CAD) systems have been proposed to integrate
the MR information. However, no comparison has been made
to find out which system performs better. In this study,
we evaluate the performance of four widely used
classifiers using leave-one-out (LOO) method. MLP and
SVM classifiers which have been successfully applied in
many branches of medical diagnostics seem promising
here. Because of their abilities to resolve nonlinear
complex relations among input variables, without the
need for any prior assumptions about these relations,
MLP and SVM models are more advisable for PCa detection.
|
1065. |
Handling missing DCE data
in prostate cancer detection using multiparametric MRI
Hussam Al-Deen Ashab1, Piotr Kozlowski1,
Robert Rohling1, Purang Abolmaesumi1,
Larry Goldenberg1, and Mehdi Moradi1
1University of British Columbia, Vancouver,
BC, Canada
The objective of the work presented here is to design
classifiers to detect prostate cancer from MRI
parametric maps with the capability of handling missing
data, specifically DCE parameters. We propose two
different methods and show their effectiveness in
maintaining high AUC while handling missing parameters.
Both methods are based on support vector machine
classification. However, one method trains a single
classifier and uses k-nearest neighbor imputation of DCE
parameters in test cases where DCE is missing. The other
method uses two different classifiers trained on DTI and
DCE, fuses the two methods in cases where both DTI and
DCE are available. We showed that as an increasing
number of cases with missing DCE features are presented
to the classifiers, KNN imputation of missing features
outperforms the fusion of two classifiers. Both methods
outperform a DTI only classifier.
|
1066. |
Pixel-Wise Multi-Parametric
Assessment of Prostate Cancer from Co-registered regions of
Pathologically defined Disease.
Chaitanya Kalavagunta1, Xiangmin Zhou2,
Stephen Schmechel3, Joseph S Koopmeiners4,
Christopher A Warlick5, Badrinath Konety5,
and Gregory J Metzger1
1Center of Magnetic Resonance Research,
University of Minnesota, Minneapolis, Minnesota, United
States, 2Center
for Research in Education and Simulation Technologies
(CREST), University of Minnesota, Minnesota, United
States, 3Department
of Laboratory Medicine and Pathology, University of
Minnesota, Minnesota, United States,4Division
of Biostatistics, School of Public Health, University of
Minnesota, Minnesota, United States, 5Institute
for Prostate and Urologic Cancers, University of
Minnesota, Minnesota, United States
Our study shows the combined power of the
multiparametric MRI parameters in the detection of
prostate cancer and their association with grade. These
results are highly unique and relevant as 1) Region of
interest (ROI) definitions were dictated by registered
pathology regions and not by manual interpretations of
pathologically identified disease and 2) pixel-wise
analysis was performed as opposed to the use of summary
statistics from within the ROIs. Performing a pixel-wise
analysis allows the apparent non-coincidence of some of
the quantitative MR parameters to be investigated. We
propose this approach is a more appropriate way to apply
predictive models moving forward.
|
1067. |
Multiparametric MRI to
Differentiate High-Risk From Low-Risk Prostate Cancer
Olga Starobinets1, Jeffry Simko2,3,
Kyle Kuchinsky2, John Kornak4,
John Kurhanewicz1,5, Dan Vigneron1,5,
Peter Carroll3, Kirsten Greene3,
and Susan Noworolski1,5
1Graduate Group in Bioengineering, University
of California, San Francisco and Berkeley, San
Francisco, CA, United States, 2Pathology,
University of California, San Francisco, CA, United
States, 3Urology,
University of California, San Francisco, CA, United
States, 4Epidemiology
and Biostatistics, University of California, San
Francisco, CA, United States, 5Radiology
and Biomedical Imaging, University of California, San
Francisco, CA, United States
The purpose of this study was to use semi-quantitative
and pharmacokinetically modeled parameters derived from
dynamic contrast-enhanced (DCE) MRI, diffusion MR and
MRI to differentiate high-risk from low-risk prostate
cancers using digitally aligned whole-mount pathology as
the standard of reference. High-risk prostate cancer had
significantly lower ADC (p<0.05) and washout slope
(p<0.05) than low-risk prostate cancer. A logistic
regression combination of parameters provided improved
discrimination (AUC=0.95). Without ADC, a combined model
yielded AUC of 0.87 for discriminating high versus low
risk prostate cancer.
|
1068. |
Correlating
multi-parametric MRI with Gleason score in human prostate
cancer
Heling Zhou1, Rami R Hallac2, Qing
Yuan1, Yao Ding3, Franto Francis4,
Robert D Sims1, Ganesh Raj5, and
Ralph P Mason1
1Radiology, University of Texas Southwestern
Medical Center, Dallas, TX, United States, 2Analytical
Imaging and Modeling Center, Children's Medical Center,
Dallas, TX, United States, 3Imaging
Physics, University of Texas MD Anderson Cancer Center,
Houston, TX, United States, 4Pathology,
University of Texas Southwestern Medical Center, Dallas,
TX, United States, 5Urology,
University of Texas Southwestern Medical Center, Dallas,
TX, United States
Prostate cancer remains the most common malignant tumor
in men. Hypoxia is an important prognostic biomarker. In
this study, 10 patients with biopsy confirmed prostate
cancer underwent MRI studies including oxygen enhanced
(BOLD and TOLD), DCE, and diffusion weighted MRI. The
multi-parametric maps were intercorrelated and compared
with Gleason score. ADC and R2* were found to
be significantly different from normal prostate and
showed general trends of decrease with higher Gleason
score. A multi-parametric approach is feasible and
provides insights into tumor pathophysiology.
|
1069. |
Prostate cancer detection
from contrast enhanced T1 time course without
pharmacokinetic modeling
Nandinee Fariah Haq1, Piotr Kozlowski2,3,
Edward C. Jones4, Silvia D Chang3,
Larry Goldenberg2, and Mehdi Moradi1
1Electrical and Computer Engineering,
University of British Columbia, Vancouver, BC, Canada, 2Urologic
Sciences, University of British Columbia, Vancouver, BC,
Canada,3Radiology, University of British
Columbia, Vancouver, BC, Canada, 4Pathology
and Laboratory Medicine, University of British Columbia,
University of British Columbia, Vancouver, BC, Canada
In this work, we propose a data-driven approach to
characterizing T1 time course. This method which is free
of physiologic modeling is used to classify prostate
tissue into cancer and normal, based on dynamic contrast
enhanced T1-weighted images. The reference standard is
the wholemount histopathologic analysis of extracted
prostate specimens. Our approach is to design a learning
agent that can detect cancer directly from the T1 time
course without modeling the physical phenomenon. The
dimensionality of the T1 time course is reduced using
Principal Component Analysis (PCA) and the resulting
parameters are used with Support Vector Machine
Classification (SVM). An area under ROC of 0.87 is
reported in pixel level classification.
|
1070. |
Comparison of an inflatable
single loop and rigid dual channel endorectal coil for
prostate imaging at 3T.
Thiele Kobus1,2, Andriy Fedorov1,
Vera Kimbrell1, Tina Kapur1,
Robert Mulkern3, and Clare Tempany1
1Radiology, Brigham and Women's Hospital,
Boston, MA, United States, 2Radiology,
Radboud University Nijmegen Medical Centre, Nijmegen,
Netherlands, 3Radiology,
Children's Hospital, Boston, MA, United States
In this study, an inflatable single loop and rigid dual
channel endorectal coil were compared for prostate
imaging at 3T. Twenty-two patients were included and T1
weighted images were used for a SNR analysis. At close
distances from the coil, the SNR in the prostate was
higher for the rigid coil compared to the inflatable
coil. The increase in SNR may be used to increase the
spatial resolution of T2 weighted images, though in this
study the 2.4 fold increase in in-plane spatial
resolution led to image quality metrics somewhat less
than those found with the inflatable coil.
|
1071. |
The Effect of Varying
Diffusion-Encoding Gradient Strength and Separation on
Measured Apparent Diffusion Coefficient and T2 of Prostate
Shiyang Wang1, Yahui Peng1,2,
Milica Medved1, Steffen Sammet1,
Ambereen Yousuf1, Weiwei Du1,3,
Yulei Jiang1, Gregory S. Karczmar1,
and Aytekin Oto1
1Department of Radiology, University of
Chicago, Chicago, IL, United States, 2School
of Electronic and Information Engineering, Beijing
Jiaotong University, Bejing, China,3Department
of Information Science, Kyoto Institute of Technology,
Kyoto, Japan
Hybrid DWI and T2 measurements showed improved contrast
enhancement in prostate cancer diagnosis. The measured
apparent diffusion coefficient can be affected by
restricted diffusion, depending on the diffusion
gradient separation (Δ). The effect of diffusion
gradient strength (g) and Δ on prostate cancer diagnosis
is unknown. Current study was performed in order to test
whether acquisitions with longer Δ are affected by
restricted diffusion. ADC/T2s obtained with hybrid DWI
sequences with fixed and non-fixed Δs were compared and
no significant differences were found. Thus restricted
diffusion does not affect the ADC values at the Δ values
used in hybrid imaging.
|
1072. |
Triexponential function
analysis on diffusion-weighted MRI in diagnosing prostate
cancer
Yu Ueda1, Satoru Takahashi2, Naoki
Ohno3, Katsusuke Kyotani1,
Nobukazu Aoyama1, Hideaki Kawamitsu1,
Yoshiko Ueno2, Kazuhiro Kitajima2,
Fumi Kawakami4, Tomoyuki Okuaki5,
Toshiaki Miyati3, and Kazuro Sugimura2
1Division of Radiology, Kobe University
Hospital, Kobe, Hyogo, Japan, 2Department
of Radiology, Kobe University Hospital, Kobe, Hyogo,
Japan, 3Faculty
of Health Sciences, Institute of Medical,
Pharmaceutical, and Health Sciences, Kanazawa
University, Kanazawa, Ishikawa, Japan, 4Department
of Diagnostic Pathology, Kobe University Hospital, Kobe,
Hyogo, Japan, 5Philips
Healthcare Asia Pacific, Minato-ku, Tokyo, Japan
To evaluate the clinical usefulness of triexponential
function analysis of diffusion weighted MRI for the
prostate cancer in the peripheral zone (PZ), we analyzed
three diffusion coefficients (Dp, Df, Ds) and fractions
(Fp, Ff, Fs), and compared them with the extra- and
intracellular component information measured with the
histopathological specimens and pharmacokinetic
parameters calculated with DCE-MRI. Triexponential
analysis would provide more detailed information on
diffusion and perfusion of prostate cancer
noninvasively. Moreover, our findings suggested that the
reduction of ADC in PZ cancer would be due to the
decrease of Ds that reflects intracellular diffusion.
|
1073. |
Diffusion-weighted imaging
of prostate cancer using statistical model based on a gamma
distribution
Hiroshi Shinmoto1, Chiharu Tamura1,
Shigeyoshi Soga1, Teppei Okamura1,
Kentaro Yamada1, Tatsumi Kaji1,
and Koichi Oshio2
1Radiology, National Defense Medical College,
Saitama, Japan, 2Diagnostic
Radiology, Keio University, School of Medicine, Tokyo,
Japan
The purpose of this study was to investigate the
distribution of diffusion coefficients in prostate
cancer (PC) and healthy peripheral zone (PZ) using the
statistical model based on a gamma distribution.
Twenty-six patients with PC were included in this study.
The mean and the standard deviation were significantly
lower in PC than in PZ. ADC < 1.0 (%) was significantly
higher in PC than in PZ and ADC > 3.0 (%) was
significantly lower in PC than in PZ. The statistical
model provides additional insight for DWI and allows us
better correlation of diffusion signal decay and
histologic findings.
|
1074. |
Quantitative DTI
Tractography of prostate gland in prostate cancer patients
Alexey A Tonyushkin1,2, Sandeep S Hedgire1,
Peter F Hahn1, Shahin Tabatabaei1,
Mukesh G Harisinghani1, and Andrew JM
Kiruluta1,2
1Radiology Dept., Massachusetts General
Hospital, Harvard Medical School, Boston, MA, United
States, 2Physics
Dept., Harvard University, Cambridge, MA, United States
Diffusion tensor imaging (DTI) is commonly used to
perform tractography that allows visualizing neuronal
fiber map in a brain. This technique seldom been used
for other visceral organs. We applied DTI tractography
to prostate MRI and developed a quantitative approach
that is able to discriminate tumor vs. normal tissue for
diagnostic purposes. We carried out HIPPA compliant
retrospective study of N=25 men with biopsy proven
prostate cancer. The results imply differences in tract
number in tumor vs. normal gland. Since these
differences are statistically significant we can design
a novel imaging tool to determine aggressiveness of
tumor during diagnostics.
|
1075. |
Rotating Frame Relaxation
Measurements in Prostate Cancer Model
Hanne Hakkarainen1, Ivan Jambor2,
Matti Poutanen3, Heidi Liljenbäck2,3,
Helena Ahtinen2, Anne Roivainen2,3,
Heikki Minn4, Miika Martikainen1,
and Timo Liimatainen1
1A.I. Virtanen Institute for Molecular
Sciences, University of Eastern Finland, Kuopio,
Finland, 2Turku
PET Centre, University of Turku, Finland, 3Turku
Center for Disease Modeling, University of Turku, Turku,
Finland, 4Department
of Oncology and Radiotherapy, Turku University Hospital,
Turku, Finland
Rotating frame relaxation times TRAFF2, TRAFF4,
T1ρ,CW, T1ρ,adiab and
T2ρ,adiab were
measured in subcutaneous prostate cancer (PC3-RFP)
tumors in several time points. The data obtained serve
as baseline of relaxation time constants for upcoming
anticancer therapy follow up using the same animal
model.
|
1076. |
Aggressiveness Biomarker
for Prostate Cancer in ADC-T2W MR Feature Space
Alpay Özcan1, Baris Türkbey2,
Peter Choyke2, and Seong K. Mun1
1Virginia Polytechnic Institute and State
University, Arlington, VA, United States, 2National
Cancer Institute, Bethesda, MD, United States
Accurate localization of prostate cancer (PCa) is
fundamental for effective surveillance and, guiding
diagnostic and therapeutic interventions. However, an
imaging biomarker is absent for this goal. Herein, the
ADC-T2W MR feature space (MR-FS) is proposed for image
guided PCa strategies. An interactive in-house software
was implemented to incorporate objectively and directly
physician's experience into the discovery process. The
analysis of a 44 patient cohort revealed a specific
region in MR-FS distinguishing aggressive from indolent
PCa. By observing the pixels associated with the
aggressive region, effective biopsy and therapy target
localization and, active surveillance is achieved.
|
1077. |
Track Density Imaging for
High Resolution Diffusion Tractography in the Prostate With
and Without Tumor
Michael Ohliger1, Cornelius Von Morze1,
Antonio Westphalen1, Natalie Korn1,
Christopher Hess1, Daniel Vigneron.1,
and John Kurhanewicz1
1Radiology and Biomedical Imaging, University
of California San Francisco, San Francisco, CA, United
States
Track density imaging of the prostate with isotropic 300
μm resolution was implemented at 3T. Imaging time was
nearly identical to a clinical diffusion-weighted
acquisition. A total of 19 patients have been imaged to
date. At least two examples are seen of tumor
interrupting tracks within the central gland. Further
work will include pathologic validation to assess the
physical basis of observed tracks.
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|
|
TRADITIONAL
POSTER SESSION ○ CANCER |
Cancer: Cells, Biopsies & Biofluid
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
|
|
1078. |
Principal component
directed partial least squares analysis for differentiation
of benign and malignant canine breast cancer: HR-MAS NMR
spectroscopy-based metabolomic study
Sang-Young Kim1, Taehyeong Lee2,
Hyunju Kim3, Eunjung Bang3,
Hwi-Yool Kim2, and Bo-Young Choe1
1Department of Biomedical Engineering, The
Catholic University of Korea, Seoul, Seoul, Korea, 2Department
of Veterinary Surgery, Konkuk University, Seoul, Korea, 3Korea
Basic Science Institute, Seoul, Korea
In this study, we aimed to evaluate the potential use of
HR-MAS NMR spectroscopy on intact tissue specimens as a
tool for prediction of canine breast cancer malignancy
through multivariate statistical analysis. HR-MAS MR
spectra of surgically obtained three types (control,
benign, malignant) of breast tissues were acquired.
Metabolic profiles were examined using the multivariate
statistical model (principal components analysis and
orthogonal signal correction pretreated partial least
square-discriminate analysis). Our findings demonstrated
that PCA directed OSC-PLS-DA analysis using 1H HR-MAS MR
metabolic profiles of breast tissues might be an
effective diagnostic and prognostic tool for the
treatment of breast cancer.
|
1079. |
Metabolic profiling of
Urinary Bladder Carcinoma Tissues by HRMAS NMR spectroscopy
Abhinav Arun Sonkar1, Shatakshi Srivastava2,
Raja A Roy2, Yadvendr A Dheer1,
and Nuzhat A Husain3
1Surgery, King George's Medical University,
Lucknow, Uttar Pradesh, India, 2Center
for Biomedical research, SGPGI, Lucknow, Uttar Pradesh,
India, 3Pathology,
RMLIMS, Lucknow, Uttar Pradesh, India
In the present work, proton HR-MAS NMR spectroscopic
studies of muscle non-invasive Urinary Bladder Carcinoma
(UBC) tissue specimens with simultaneous urine analysis
has been performed. The detailed metabolic profiling
demonstrated significant presence of taurine and
branched chain amino acids (BCAA) in tissues of 24
patients suffering from superficial UBC when compared
with 29 tissue specimens from the same subjects with
non-malignant biopsies. The proton NMR spectra were then
subjected to PCA and PLS-DA multivariate analysis. The
validated model allowed >85% correct classification of
malignant tissues when compared with gold standard
histopathological examinations.
|
1080. |
Metabolic characterization
of locally advanced breast cancer in response to NAC
treatment
Shiva Shojaei Moghaddam1, Maria D. Cao1,
Guro F. Giskeødegård1, Hans E. Fjøsne1,
Steinar Lundgren1, Per E. Lønning2,
and Tone F. Bathen1
1NTNU, Trondheim, Sør-Trøndelag, Norway, 2University
of Bergen, Begren, Norway
Metabolic profiling has shown promise in breast cancer
characterization. High resolution magic angle spinning
MR spectroscopy was performed on biopsies obtained
before and after neoadjuvant chemotherapy in patients
with locally advanced breast cancer. Quantitative
metabolite concentrations were related to the treatment
response and survival of the patients.
Glycerophosphocholine, Glycine and myo-Inositol showed
significant changes in response to NAC treatment among
survivors, responders and non-responders. Findings from
this study indicate that the MR metabolic profile in
response to NAC treatment can assist the prediction of
prognosis and clinical treatment response in LABC
patients.
|
1081. |
NMR spectroscopy identifies
two subtypes with different metabolic profiles in stem-like
cells from Glioblastoma multiforme
Alessandra Palma1, Sveva Grande1,
Anna Maria Luciani1, Antonella Rosi1,
Mauro Biffoni2, Lucia Ricci-Vitiani2,
Daniele Runci2, Roberto Pallini3,
Vincenza Viti4, and Laura Guidoni4
1Dipartimento di Tecnologie e Salute,
Istituto Superiore di Sanità and INFN Sanità Group,
Roma, Italy, Italy, 2Dipartimento
di Ematologia, Oncologia e Medicina Molecolare, Istituto
Superiore di Sanità, Italy, Italy, 3Dipartimento
di Neurochirurgia, Università Cattolica del Sacro Cuore,
Roma, Italy, Italy, 4INFN
Sanità Group, Roma, Italy, Italy
Recurrence of the glioblastoma after conventional
treatments is attributed to the overgrowth of stem-like
cancer cells resistant to treatments. 1H NMR spectra run
on glioblastoma derived stem-like cells grown in
neurospheres showed intense signals common in brain and
brain tumours including NAA, creatine, myoinositol,
glutamine and neutral lipids. Unsupervised cluster
analysis performed on spectral data of cells from 27
glioblastoma patients identified two different NMR-based
groups with different metabolism. A mixed neural–astrocyte
metabolic phenotype with a strong neuronal fingerprint
prevailed in one group (15 cell lines) and an astrocytic/glioma-like
metabolism was prevalent in the other cluster (12 cell
lines).
|
1082. |
Metabolic profile of human
breast tissues studied by in-vitro NMR spectroscopy
Naranamangalam R Jagannathan1, Rani G Sah1,
Uma Sharma1, Rajinder Parshad2,
and Vurthaluru Seenu2
1Department of NMR & MRI Facility, All India
Institute of Medical Sciences, New Delhi, Delhi, India, 2Department
of Surgical Disciplines, All India Institute of Medical
Sciences, New Delhi, Delhi, India
High-resolution in-vitro NMR spectroscopy was used to
determine the absolute concentration of various
metabolites in 23 breast tissues, both involved (n=11)
and non-involved (n=13). One-dimensional and two-
dimensional NMR experiments (DQF-COSY and TOCSY) were
carried out at 400.13 MHz. The concentration of Lactate
(14.0 ± 11.8 mmol/kg), Creatine (1.9 ± 1.2 mmol/kg),
Choline (3.1 ± 2.2 mmol/kg), Glycerophosphocholine/Phosphocholine
(5.2 ± 4.1 mmol/kg) and Glutamate/Glutamine (8.3 ± 5.4)
mmol/kg in involved tissues were significantly higher
compared to non-involved tissues, indicating a general
increase in the metabolic activity in tumor tissues and
thus providing an insight into the tumor metabolism.
|
1083. |
Phospholipid metabolism,
but not energy metabolism is affected by expression of the
multidrug resistance transporter ABCB5 in G3361 melanoma
stem cells
Norbert W Lutz1, Jie Ma2, Patrick
J Cozzone1, and Markus H Frank2
1CRMBM, Faculté de Médecine, Aix-Marseille
University, Marseille, France, 2Transplant
Research Program, Boston Children’s Hospital, Harvard
Medical School, Boston, MA, United States
|
1084. |
The effect of choline
kinase-α inhibition on lipid metabolism of breast cancer
cells
Noriko Mori1, Flonné Wildes1,
Kristine Glunde1, and Zaver M. Bhujwalla1
1The Russell H. Morgan Department of
Radiology and Radiological Science, The Johns Hopkins
University School of Medicine, Baltimore, Maryland,
United States
Phosphatidylcholine has important roles in membrane
structure and cell signaling. Increased levels of
choline kinase (Chk)-α and phosphocholine (PC) are
consistently observed in aggressive cancers.
Understanding the roles of Chk-α in cancer can result in
new therapies. We previously showed that the Chk-α
protein, but not PC was essential for cell survival of
two triple negative breast cancer cell lines, MDA-MB-231
and SUM149, using a Chk-α inhibitor which reduces PC but
not Chk-α protein. Here we have investigated lipid
metabolism in these breast cancer cells and identified
PtdCho as an important factor in breast cancer cell
survival.
|
1085. |
Metabolic Analysis of
Slowly Cycling Melanoma Cells
Sergey Magnitsky1 and
Geetha Mohan1
1Radiology and Biomedical Imaging, University
of California San Francisco, San Francisco, California,
United States
Low efficacy of existing treatment for various human
cancers has been attributed to the existence of cancer
stem cells. Such slowly cycling sub-population of cells
in melanoma exhibits high tumorigenicity, self-renewal
capacity and drug resistance. The goal of this study was
to delineate metabolic differences between slowly
cycling sub-population and bulk tumor cells.
Ethanol/chloroform cells extracts were prepared from
sorted cells. High-resolution NMR spectra were acquired.
NMR data revealed high intracellular lactate and choline
concentration in slowly cycling sub-population cells
compared to fast cycling tumor cells. Approximately 70%
of lactate produced in unsorted cells was produced by
slowly cycling sub-population.
|
1086. |
Role of Choline Kinase and
Ethanolamine Kinase Isoforms in Modulating
Phosphoethanolamine Levels in Breast Cancer Cells
Tariq Shah1, Balaji Krishnamachary1,
Flonne Wildes1, Jannie Wijnen2,
Kristine Glunde1, and Zaver M Bhujwalla1
1Division of Cancer Imaging Research,
Department of Radiology, Johns Hopkins University,
Baltimore, Maryland, United States, 2Cancer
center, University Medical Centre Utrecht, Utrecht,
Netherlands
While significant effort has been focused on the
increased phosphocholine (PC) levels observed in cancer
cells and tumors, increased phosphoethanolamine (PE) has
been underexplored. Increased PC, but not PE, is
observed in cells in culture because culture medium
contains free choline, but no ethanolamine. We have used
siRNAs to silence specific genes involved in choline and
ethanolamine metabolism to understand their roles in
intracellular metabolite levels measured with
high-resolution phosphorus MR spectroscopy of cell
extracts. We have demonstrated that both Chk-α and
EthnK1 contribute to PE levels observed in vivo with the
latter having a primary role in its biosynthesis.
|
1087. |
CEST imaging of human
breast cancer cells
Catherine DeBrosse1, Mohammad Haris1,
Ravi Prakash Reddy Nanga1, Hari Hariharan1,
Damodar Reddy1, Imran Mohammad2,
Kejia Cai1, Anup Singh1, and
Ravinder Reddy1
1Center for Magnetic Resonance and Optical
Imaging, Department of Radiology, University of
Pennsylvania, Philadelphia, Pennsylvania, United States, 2Department
of Pharmacology and Institute for Translational Medicine
and Therapeutics, University of Pennsylvania,
Philadelphia, Pennsylvania, United States
The purpose of this study was to determine feasibility
of glutamate chemical exchange saturation transfer
(GluCEST) imaging in human breast cancer cell lines
treated with poly-L-glutamate (PLG). PLG has been used
as a drug-conjugate in recently developed cancer
therapies, as it is broken down by tumor proteases.
Glutamate fragments that result from PLG degradation
have labile amine protons that exchange with water and
give GluCEST signal. In this study, we demonstrate that
treatment of human breast cancer cells with PLG led to
an increase in GluCEST signal due to the breakdown of
PLG by tumor proteases such as cathepsins.
|
1088. |
The effect of
aminooxyacetate on metabolism of breast cancer cells
Noriko Mori1, Preethi Korangath2,
Santosh Bharti1, Flonné Wildes1,
Saraswati Sukumar1,2, and Zaver M. Bhujwalla1,2
1The Russell H. Morgan Department of
Radiology and Radiological Science, The Johns Hopkins
University School of Medicine, Baltimore, Maryland,
United States, 2The
Sidney Kimmel Comprehensive Cancer Center, The Johns
Hopkins University School of Medicine, Baltimore,
Maryland, United States
Aminooxyacetate (AOA) is a known inhibitor of the
transamination reaction. We previously found that AOA
treatment showed dose dependent growth inhibitory
activity in breast cancer cells, especially in glutamine
dependent cancer cells such as SUM159. To investigate
the mechanism of AOA action, we used 1H MRS of cell
extracts and conditioned media from SUM159 and observed
reductions of alanine, aspartate, phosphocholine, and
increases of glutamate and tyrosine following treatment
with 2mM AOA for 24h. Lactate production and glucose
consumption in conditioned media and the level of Chk-α
that catalyzes the formation of phosphocholine were not
affected by AOA.
|
1089. |
Role of Lymphatic
Endothelial Cells in Prostate Cancer Cell Invasion in Tumor
Microenvironments
Tariq Shah1, Flonne Wildes1,
Dmitri Artemov1, and Zaver M Bhujwalla1
1Division of Cancer Imaging Research,
Department of Radiology and Radiological Sci, Johns
Hopkins University, Baltimore, Maryland, United States
While the presence of lymph node metastasis as a major
prognosticator for many cancers, including prostate
cancer, is well established, the regulation of
tumor-associated lymphangiogenesis and the
microenvironmental factors that affect the invasion of
cancer cells into lymphatic vessels requires additional
investigation. Here we have investigated the role of
lymphatic endothelial cells prostate-cancer cell
interaction in the invasion and degradation of the
extracellular matrix (ECM) under normoxic and hypoxic
environments using our MR compatible cell perfusion
assay, and determined the associated metabolic changes.
|
|
|
TRADITIONAL
POSTER SESSION ○ CANCER |
Tumor Perfusion & Permeability: Applications
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
|
|
1090. |
Initial experience:
combination of MR pharmacokinetic modeling and FDG uptake
using simultaneous dynamic contrast enhanced MRI and PET
imaging
Nathaniel E. Margolis1, Linda Moy1,
Akshat C. Pujara1, Alana Amarosa1,
Eric E. Sigmund1, Christian Geppert2,
Christopher Glielmi2, Melanie Freed1,
Li Feng1, Ricardo Otazo1, Amy N.
Melsaether1, and Sungheon Kim1
1Radiology, NYU Langone Medical Center, New
York, New York, United States, 2Siemens
Medical Solutions, New York, New York, United States
The objective of our study was to assess the feasibility
of using DCE-MRI and PET data for the assessment of
breast cancer MR pharmacokinetics and metabolic
activity. A whole-body integrated 3 T PET/MR scanner was
used to simultaneously acquire DCE-MRI and PET images of
the breast in the prone position. We found trends
between DCE-MRI kinetic model parameters, metastatic
burden, and progesterone receptor status. Our
preliminary results demonstrate the feasibility of using
simultaneous acquired DCE-MRI and PET measures for
better characterization of breast lesions.
|
1091. |
Simulation analysis of
region-of-interest measurement errors on parameter maps
derived from Dynamic Contrast-Enhanced MRI and T1 mapping of
small volume breast cancer
Moira C Schieke1
1Lakeshore, Milwaukee, WI, United States
|
1092. |
Evidence of intra-patient
and inter-patient heterogeneity in the microvasular
characteristics of colorectal cancer liver metastases
Laura Horsley1, Neil Thacker2,
Ross Little3, Yvonne Watson3, Sue
Cheung3, Geoff Parker3, Gordon
Jayson1, and Alan Jackson2
1Institute for Cancer Studies Christie
Hospital NHS Foundation Trust, University of Manchester,
Manchester, United Kingdom, 2Wolfson
Molecular Imaging Centre, University of Manchester,
Manchester, Greater Manchester, United Kingdom, 3Centre
for Imaging sciences & Biomedical Imaging Institute,
University of Manchester, United Kingdom
This study used DCE-MRI to compare the microvascular
characteristics of liver secondaries in patients with
advanced colorectal cancer. We particularly wished to
demonstrate whether differences could be detected
between liver secondaries in the same patient or between
liver secondaries in different patients, using standard
DCE-MRI techniques employed for clinical trials. In
order to test this hypothesis we developed a statistical
method which incorporated information on the measurement
reproducibility and error for median values of
parameters Ktrans, ve, vp, EF and ADC. There was more
variability between liver secondaries in different
patients than there was between secondaries in the same
patient.
|
1093. |
Extramural Depth of Tumor
Invasion at Thin-Section MR in Rectal Cancer: associating
with prognostic factors and ADC value
Tong Tong1, Yajia Gu2, Weijun Peng2,
and He Wang3
1Cancer Hospital, Shanghai, Shanghai, China, 2Cancer
Hospital, Shanghai, China, 3MR
Research China, GE Healthcare, Shanghai, China
To assess the value of maximal extramural depth (EMD) of
T3 tumor spread on MRI as a potential noninvasive
imaging biomarker of tumor aggressiveness in rectal
cancer.Tumor EMDs differ between CEA <5 ng/mL versus¡Ý5
ng/mL(P=0.013), CA19-9<27U/mL versus¡Ý27 U/mL(P=0.012) ,
the groups of cN0 versus cN+ cancers (P=0.049), and
between the several groups of histological
differentiation grades (P=0.033).A significant negative
correlation (r=-0.581; P=0.001) between ADC and EMD
values was found. Significant correlations were found
between EMD values and CEA,CA19-9 level, differentiation
grade and ADC value. EMD has the potential to become an
imaging biomarker of tumor aggressiveness profile.
|
1094. |
Pulsed-continuous arterial
spin labeling MRI with multiple post-labeling delay in renal
cell carcinoma: clinical feasibility and initial results of
a comparative study with parametric dynamic
contrast-enhanced MRI
Nobuyuki Kosaka1, Katsuki Tsuchiyama2,
Kazuhiro Shimizu1, Yasuhiro Fujiwara3,
Tsuyoshi Matsuda4, Tatsuya Yamamoto1,
Tatsuro Tsuchida1, Nobuyuki Oyama2,
and Hirohiko Kimura1
1Department of Radiology, University of
Fukui, Eiheiji, Fukui, Japan, 2Department
of Urology, University of Fukui, Eiheiji, Fukui, Japan, 3Radiological
Center, University of Fukui Hospital, Eiheiji, Fukui,
Japan, 4Global
MR Applications and Workflow, GE Healthcare Japan, Hino,
Tokyo, Japan
Pulsed-continuous arterial spin labeling MRI (pcASL)
with multiple post-labeling-delay to measure arterial
transit time-corrected tumor blood flow (ATC-TBF) in
renal cell carcinoma was performed and compared to
parametric dynamic contrast-enhanced MRI (DCE-MRI). All
image acquisitions and data post-processings were
successfully achieved in all 6 patients, and high
signals of 5 clear cell carcinomas were visually
identified. Both maximum slope and contrast enhancement
ratio correlated significantly with ATC-TBF. Ktrans,
ve, and IAUGC90@showed positive
but non-significant correlations. pcASL with multiple
PLD appears clinically feasible for measuring ATC-TBF,
which correlated with several hemodynamic parameters of
DCE-MRI.
|
1095. |
Quantitative perfusion and
diffusion weighted magnetic resonance imaging of pancreatic
adenocarcinoma: a pilot study
Hyunki Kim1, Pablo Arnoletti2,
John Christein1, Marty Heslin1,
James Posey1, Amol Pednekar3, T.
Beasley1, and Desiree Morgan1
1University of Alabama at Birmingham,
Birmingham, AL, United States, 2Center
for Specialized Surgery, FL, United States, 3Philips
Medical Systems, WA, United States
Breath-hold DCE-MRI/DWI was applied for 16 patients with
treatment-naïve pancreatic adenocarcinoma. The
physiological parameters such as Ktrans, kep and ADC
values in pancreatic tumors, non-tumor adjacent
pancreatic parenchyma (NAP), liver metastases, and
normal liver tissues were quantitated. Ktrans, kep and
ADC values of pancreatic tumors were significantly lower
than those of non-tumor adjacent pancreatic parenchyma.
Thus, the perfusion and diffusion parameters may be
utilized as diagnostic markers for pancreatic cancer
detection.
|
1096. |
LOCAL VASCULAR INPUT
FUNCTION FOR PHARMACOKINETIC MODELING OF PROSTATE CANCER
Hatef Mehrabian1, Masoom A. Haider2,
and Anne L. Martel1
1Medical Biophysics, University of Toronto,
Toronto, Ontario, Canada, 2Medical
Imaging, Sunnybrook Health Sciences Centre, Toronto,
Ontario, Canada
A major component in multi-parametric MRI of tumors is
pharmacokinetic modeling of their DCE-MRI which provides
information about perfusion and vascular permeability.
Such analysis requires an AIF that is approximated
outside of the tissue and is a major source of error and
discrepancy among studies. Using a local vascular input
function (VIF) instead has the potential to improve PK
analysis. This paper investigates the effects of using
VIF (in 19 prostate DCE-MRI datasets) and shows more
consistent PK parameters are obtained for normal
peripheral zone tissue compared to using AIF and result
in better separation of tumor and normal tissues.
|
1097. |
Repeatability of DCE-MRI
Parameters in a Paediatric Oncology Population
Neil P Jerome1, Keiko Miyazaki1,
David J Collins1, Matthew R Orton1,
James d'Arcy1, Lucas Moreno2,3,
Andrew D J Pearson2,3, Lynley V Marshall2,3,
Fernando Carcellar2,3, Martin O Leach1,
Stergios Zacharoulis2,3, and Dow-Mu Koh4
1CR-UK and EPSRC Cancer Imaging Centre, The
Institute of Cancer Research, Sutton, Surrey, United
Kingdom, 2Paediatric
Drug Development Team, Cancer Therapeutics and Clinical
Studies, The Institute of Cancer Research, Sutton,
Surrey, United Kingdom, 3Paediatric
Drug Development Unit, Children and Young People's Unit,
The Royal Marsden NHS Foundation Trust, Sutton, Surrey,
United Kingdom, 4Department
of Radiology, Royal Marsden Hospital, Sutton, Surrey,
United Kingdom
It is essential that functional imaging-derived
biomarkers have acceptable repeatability in order to
have confidence in measured changes. Where paediatric
populations may exhibit varying physiology/metabolism to
adults, there is a need to specifically assess
repeatability of DCE-MRI in a paediatric population. For
a paediatric cohort (median age 11, range 6 – 15 years)
of five extra- and seven intra-cranial solid tumours,
DCE was performed on two successive days, with analysis
using cohort-derived AIF and extended Tofts model. Both
model-derived and model-independent parameters showed
acceptable repeatability (CV<20%), with native T1 and
IAUGC60 performing best (CV 6.2 % and 12.8 %
respectively).
|
1098. |
Comparison of
Patient-Specific and Fixed Arterial Input Functions for
Assessing Treatment Response at DCE-MRI
Mihaela Rata1, Matthew R Orton1,
Christina Messiou1, Elly Castellano1,
Helen Young2, Nandita de Souza1,
David J Collins1, and Martin O Leach1
1CRUK and EPSRC Cancer Imaging Centre,
Institute of Cancer Research & Royal Marsden NHS
Foundation Trust, Sutton, Surrey, United Kingdom, 2Early
Clinical Development, AstraZeneca, Macclesfield, United
Kingdom
Accurate AIF measurement in DCE-MRI studies is
challenging due to various confounding factors: in
clinical trials looking at treatment response a fixed
AIF is often used. Whilst this removes a major source of
variation, if the treatment affects the AIF, such
changes will be erroneously reflected in the tissue
parameters. This abstract compares the repeatability and
treatment effect of Ktrans obtained using three AIFs:
fixed AIF; AIF from a vessel in the DCE-MRI data; AIF
obtained on the same day with a DC-CT examination. A
fixed AIF is most repeatable, but the DC-CT AIF has a
more significant treatment effect.
|
1099. |
In Vivo Assessment of
Non-Small Cell Lung Cancer: Detection of Early Response to
Concurrent Chemoradiotherapy by Using Breath-Hold Dynamic
Contrast Enhanced MRI
Xiuli Tao1, Han Ouyang1, Feng Ye1,
Zihua Su2, Xiao Xu2, and Ning Wu1
1Cancer Hospital£¬Chinese Academy of Medical
Sciences & Peking Union Medical College, Beijing, China, 2GE
Healthcare, Beijing, China
DCE-MRI has been extensively used in monitoring
treatment response on many anatomies. However, this
technique was not fully explored in lung cancer due to
breathing motion. In this paper, we demonstrated by
using a mutual information based nonlinear registration
scheme and two compartment Tofts model, clinical
relevant parameters could be extracted from a
breath-hold DCE-MRI to monitor treatment response on
NSCLC.
|
1100. |
The response to
chemotherapy of mesothelioma tumours as assessed by dynamic
contrast-enhanced MRI: first impressions
Andrew B Gill1,2, Andrew N Priest2,
and Nagmi Qureshi1
1Radiology, Papworth Hospital NHS Foundation
Trust, Cambridge, United Kingdom, 2Medical
Physics, Cambridge University Hospitals, Cambridge,
United Kingdom
Mesothelioma has rarely been the subject of DCE-MRI
investigations. This study applies pharmacokinetic
modeling to DCE-MRI data acquired in patients with
mesothelioma tumours to generate parameters associated
with tumour perfusion (e.g. Ktrans, vp).
Results from examinations before and after chemotherapy
are reported in this abstract. Initial findings indicate
that changes in Ktrans may
correlate well with the response to treatment as
evaluated by standard CT RECIST measures. Further
patient numbers are needed to confirm these early
impressions.
|
1101. |
Model Independent Method on
Modified DCE-MRI Perfusion Data for Exploring Area and Grade
of Gliomas
Bob L Hou1, Alice B Lai2, Guodong
Guo2, and Jeffrey S Carpenter1
1Radiology, WVU, Morgantown, WV, United
States, 2Computer
and EE, WVU, Morgantown, WV, United States
A common approaching to find brain tumor area and grade
it from DCE-MRI perfusion data is to get the maps of
volume transfer constant (Ktrans) and fractional
extracellular-extravascular space volume (Ve) from
pharmacokinetic models. However there are questions on
the models, and by using the models is very difficult to
distinguish the Grade III with the Grade IV gliomas. In
this study, we sought to apply a model independent
method, i.e., Probabilistic Independent Component
Analysis (PICA), on modified DCE data for finding the
tumor areas and distinguishing their grades.
|
1102. |
ASSESSING THE EFFECTS OF
DECREASING TEMPORAL RESOLUTION ON PHARMACOKINETIC ANALYSIS
USING A LOCAL VASCULAR INPUT FINCTION
Hatef Mehrabian1, Masoom A. Haider2,
and Anne L. Martel1
1Medical Biophysics, University of Toronto,
Toronto, Ontario, Canada, 2Medical
Imaging, Sunnybrook Health Sciences Centre, Toronto,
Ontario, Canada
Pharmacokinetic (PK) analysis of tumor DCE-MRI provides
information about its vasculature. Such analysis
requires an AIF, which has a narrow temporal profile,
and its measurement requires data with high temporal
resolution (resulting in low spatial resolution images).
This paper investigates possibility of using a local
vascular input function (VIF) that has a wider temporal
profile and can be measured in low temporal resolution
datasets, in PK analysis and shows VIF-based PK
parameters are less sensitive to low temporal resolution
compared to AIF-based parameters. Lowering temporal
resolution enables imaging with high spatial resolution
which improves both VIF calculation and PK analysis.
|
1103. |
A novel and affordable
DCE-MRI phantom: experimental setup and assessment of
reproducibility
Hector Sanchez Casas1, Araminta E. W. Ledger1,
Craig Cummings1, Maria A. Schmidt1,
Martin O. Leach1, and Marco Borri1
1CR-UK and EPSRC Cancer Imaging Centre,
Institute of Cancer Research and Royal Marsden, Sutton,
Surrey, United Kingdom
DCE-MRI has an established role as both a diagnostic and
research tool. This work presents a novel DCE-MRI test
object of simple and affordable design, which can create
reproducible dynamic enhancement curves employing
commonly available automated contrast agent injectors. A
reproducible reference dynamic enhancement curve is a
valuable tool in routine QA and can be employed to
investigate the effect of MR sequence alterations on
curve shape.
|
1104. |
Adaptive spatio-temporal
resolution for accelerated (ASTRA) DCEMRI driven by
pharmacokinetic modelling
Rashmi Reddy1, Shasmshia Tabassum1,
Shaikh Imam1, Nithin N Vajuvalli1,
Sowmya Ramachandra1, and Sairam Geethanath1
1Medical Imaging Research Center, Dayananda
Sagar Institutions, Bangalore, karnataka, India
The proposed algorithm is based on an application of
compressed sensing (CS) on dynamic contrast enhancement
MRI (DCE-MRI). It involves the adaptive undersampling
technique wherein the acquisition of more number of
frames during the uptake aid to the improved Ktrans
value and the high resolution images obtained during
wash out aid in the improved Ve value. The technique is
carried out on Qiba dataset (QIBA_v7_Tofts) by using a
variable density Poisson mask for undersampling the
k-space data. The proposed algorithm reconstructs the
data by using combinations of the different acceleration
factors viz. 1X, 2X, 4X, 6X and 6X/4X, as a result of
which we are able to obtain better parametric maps with
reduction in acquisition time. The quality of the
reconstructed results is validated by calculating the
NMRSE values and parametric maps for the data with
different acceleration factors.
|
1105. |
Error Quantification in
Relaxivity Rate Change (∆R1) Due to Systematic Errors in
Dynamic Contrast Enhanced MR Studies
Hassan Bagher-Ebadian1,2, Siamak P.
Nejad-Davarani3,4, James R Ewing2,3,
and Hamid Soltanian-Zadeh1,5
1Radiology, Henry Ford Hospital, Detroit, MI,
United States, 2Physics,
Oakland University, Rochester, MI, United States, 3Neurology,
Henry Ford Hospital, Detroit, MI, United States, 4Biomedical
Engineering, University of Michigan, Ann Arbor, MI,
United States, 5CIPCE,
ECE Dept., University of Tehran, Tehran, Iran
In Dynamic Contrast Enhanced (DCE) MR studies,
assessment of systematic errors propagated in
longitudinal relaxation rate change, ∆R1(t), is
important since errors in ∆R1(t) profile, biases
permeability parameters estimated in
DCE-MR-Pharmacokinetic analysis. Herein, we asses and
quantify the biasing of ∆R1(t) profile at different
enhancement-ratios in the DCE-T1
(3D-Spoiled-Gradient-Echo) experiment. Biasing arises
from the deviation of actual-to-nominal
dynamic-flip-angle and also the systematic error in
estimating of resting T1 in Variable-Flip-Angle
experiments prior to the contrast agent administration.
Results imply that ∆R1(t), regardless of its enhancement
ratio, is more susceptible to the underestimations of T1
and dynamic-flip-angel compared to their overestimations
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|
TRADITIONAL
POSTER SESSION ○ CANCER |
Tumor Therapy Response: Clinical & Preclinical
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
|
|
1106. |
Spatial Heterogeneity
Analysis of DCE- and DW-MRI Using the Logistic Ridge
Regression to Predict Breast Cancer Response to Neoadjuvant
Therapy
Xia Li1, Hakmook Kang1, Lori R.
Arlinghaus1, A. Bapsi Chakravarthy1,
Richard G Abramson1, Vandana Abramson1,
and Thomas E Yankeelov1
1Vanderbilt University, Nashville, Tennessee,
United States
DCE- and DW-MRI have been used to predict the response
of breast tumors to neoadjuvant chemotherapy (NAC).
However, most studies quantify changes in parameters
averaged over the tumor ROI and therefore discard all
spatial information related to tissue heterogeneity. In
this study, a novel voxel-by-voxel analysis based on a
logistic ridge regression model was employed to optimize
the ability of DCE- and DW-MRI to predict the response
of breast tumors to NAC. The results indicate that
incorporating changes in the spatial heterogeneity in
DCE- and DW-MRI data improves the ability to predict
treatment response for breast cancer patients receiving
NAC.
|
1107. |
DIFFUSION WEIGHTED MRI FOR
RADIOTHERAPY TREATMENT OF LOCALLY ADVANCED CERVICAL CANCER –
TREATMENT RESPONSE ASSESSMENT USING DIFFERENT SEGMENTATION
METHODS
Søren Haack1, Kari Tanderup2,
Jesper Folsted Kallehauge3, Jacob Christian
Lindegaard2, Erik Morre Pedersen4,
and Sune Nørhøj Jespersen5,6
1Dept. of Clinical Engineering, Aarhus
University Hospital, Aarhus, Denmark, 2Dept.
of Oncology, Aarhus University Hospital, Aarhus,
Denmark, 3Dept.
of Medical Physics, Aarhus University Hospital, Aarhus,
Denmark, 4Dept.
of Radiology, Aarhus University Hospital, Aarhus,
Denmark, 5CFIN/MindLab,
Aarhus University, Aarhus, Denmark,6Dept. of
Physics and Astronomy, Aarhus University, Aarhus,
Denmark
Diffusion weighted MRI has shown great potential in
diagnostic cancer imaging and may also have value for
monitoring tumor response during radiotherapy. Before DW
MRI can be used for monitoring treatment response
objective methods for segmentation of the hyper-intense
signal of the tumor at high b-value images should be
evaluated. This study evaluates three objective
segmentation methods used for monitoring treatment
response of twelve patients with advanced cervical
cancer treated with external beam radiotherapy followed
by brachytherapy. Segmented volume, resulting mean ADC
and histogram analysis are compared and evaluated.
|
1108. |
Repeatability of
geometrically corrected DWI scans for treatment response
monitoring in oesophageal cancer
Astrid L.H.M.W. van Lier1, Peter S.N. van
Rossum1,2, Gert J. Meijer1,
Cornelis A.T. van den Berg1, Mariëlle E.P.
Philippens1, Jan J.W. Lagendijk1,
Marco van Vulpen1, and Irene M. Lips1
1Radiotherapy, UMC Utrecht, Utrecht, Utrecht,
Netherlands, 2Surgery,
UMC Utrecht, Utrecht, Utrecht, Netherlands
Prior to constructing a model for DWI-based response
prediction in esophageal cancer, we investigated the
repeatability of the ADC determination in the tumor. As
the DWI images are geometrically distorted, we opted for
retrospective correction of the maps prior to analysis.
The coefficient of repeatability was found to be 11.0%
(Bland-Altman analysis). No significant correlation was
found between the ADC repeatability error and mean pixel
shift. The repeatability error was generally smaller
than the pre-per and pre-post treatment ADC difference
(8/11 cases). We will continue to use the proposed DWI
protocol for development of a treatment response
prediction model.
|
1109. |
ADC histogram analysis:
investigation of treatment response and survival in advanced
ovarian cancer
Andrew Nicholas Priest1, Andrew J Patterson1,
Masako Y Kataoka1, Ilse Joubert1,
Mary A McLean2, Martin John Graves1,
Charlotte Hodgkin2, Robin A Crawford3,
Helena M Earl3, John R Griffiths2,
James D Brenton2,3, David John Lomas1,
and Evis Sala1
1Radiology, Addenbrooke's Hospital and
University of Cambridge, Cambridge, United Kingdom, 2Cancer
Research UK Cambridge Institute, Cambridge, United
Kingdom,3Oncology and Gynaecological
Oncology, Addenbrooke's Hospital, Cambridge, United
Kingdom
Diffusion-weighted imaging was used to assess treatment
response in advanced ovarian cancer. Histogram analysis
can potentially give more information about
heterogeneous tumours than mean values. This study
investigated, for both primary ovarian tumours and
metastatic disease, how ADC histogram parameters change
with neoadjuvant chemotherapy, and their relationships
to treatment response and survival. Highly significant
changes were found for the primary tumour in responders
but not non-responders, with significantly greater
changes in responders for the mean, 75th and 90th
percentiles. However, no significant differences or
changes were found for metastatic lesions. No
relationship with survival was found for any lesion.
|
1110. |
Functional Diffusion
Mapping (fDM) for Quantitative DW-MRI to Predict Breast
Cancer Response to Neoadjuvant Chemotherapy
Xia Li1, Lori R Arlinghaus1, A
Bapsi Chakravarthy1, Richard G Abramson1,
Vandana Abramson1, and Thomas E Yankeelov1
1Vanderbilt University, Nashville, Tennessee,
United States
DW-MRI has been used to predict treatment response in
breast cancer. Studies have shown the ability of the
functional diffusion mapping (fDM) method applied on DW-MRI
as an early biomarker for survival for patients with
brain tumor. However, there is only one study reporting
the fDM analysis on breast cancer data. In this study,
we attempted to determine 1) if fDM performed on
patients with breast cancer can be used to separate
responders from non-responders, and 2) does the fDM
approach outperform simple region of interest based
analysis. The results indicate that the fDM approach on
the DW-MRI breast data retains the information of tumor
heterogeneity, therefore allowing for an improved
ability to predict treatment response when compared to a
standard region of interest based analysis.
|
1111. |
1.0T MR-based Treatment
Planning for Spinal Stereotactic Radiosurgery – Initial Case
Study
Ning Wen1, Joshua Kim1, Carri
Glide-Hurst1, Bo Zhao1, Yimei
Huang1, David Hearshen2, Milan
Pantelic2, M.Salim Siddiqui1,
Kenneth Levin1, Benjamin Movsas1,
Indrin Chetty1, and Samuel Ryu1
1Radiation Oncology, Henry Ford Health
System, Detroit, Michigan, United States, 2Radiology,
Henry Ford Health System, Detroit, Michigan, United
States
This study is to investigate the feasibility of
developing a stereotactic radiosurgery treatment
protocol for spinal metastatic lesions based solely on a
dedicated 1.0 T magnetic resonance simulation platform.
The dose was calculated on a synthetic CT image set
generated from a weighted combination of T1-weighted and
T2-weighted images for one patient. The dose calculation
difference between CT and synthetic CT was within 3%.
However, the bony segmentation, metal artifacts and
geometric distortion correction need to be further
investigated to use MRI as the primary imaging modality
for spinal radiosurgery.
|
1112.
|
T1ρ Mapping
for the Evaluation of High Intensity Focused Ultrasound
Tumor Treatment
Stefanie JCG Hectors1,2, Rik PM Moonen1,2,
Gustav J Strijkers1,2, and Klaas Nicolay1,2
1Biomedical NMR, Department of Biomedical
Engineering, Eindhoven University of Technology,
Eindhoven, Netherlands, 2Center
for Imaging Research and Education, Eindhoven,
Netherlands
This study was aimed to assess the effects of HIFU
treatment on tumor T1ρ. T1ρ measurements
at various spin-lock amplitudes (0-2000 Hz) were
performed before, directly after and 3 days after HIFU
treatment of murine tumors. The tumor T1ρ at
spin-lock amplitudes higher than or equal to 100 Hz
significantly decreased at 3 days after HIFU compared to
pre-treatment. The T1ρ decline
after HIFU became significantly larger with increasing
spin-lock amplitudes, indicative of increased contrast
between HIFU-treated and non-treated tissue at higher
spin-lock amplitudes. Altogether, the data suggest that
T1ρ is
a suitable biomarker for the evaluation of HIFU
treatment.
|
1113. |
Monitoring therapeutic
effect of a vascular disrupting agent: correlation between
perfusion parameters derived from intravoxel incoherent
motion diffusion-weighted imaging and dynamic contrast
enhanced MRI
Ijin Joo1, Jeong Min Lee1, Joon
Koo Han1, and Byung Ihn Choi1
1Seoul National University Hospital, Seoul,
Seoul, Korea
Dynamic contrast enhanced (DCE) MRI has been widely used
for noninvasive assessment of the change in tumor
perfusion. Recently, intravoxel incoherent motion (IVIM)
diffusion-weighted imaging (DWI) by using a
bi-exponential fitting of the DWI data from multiple
b-values has been reported to be useful for quantitative
measurement of tumor perfusion without requirement of
contrast medium. Our study using a rabbit liver tumor
model demonstrated significant correlation between
serially measured perfusion parameters derived from
IVIM-DWI and DCE-MRI in the vascular disrupting agent
(VDA)-treated group. Therefore, IVIM-DWI may be a useful
surrogate of DCE-MRI in the longitudinal monitoring
therapeutic effect of VDAs.
|
1114. |
Targeting choline
phospholipid metabolism: GDPD5 and GDPD6 silencing decreases
breast cancer cell proliferation and invasion
Maria Dung Cao1,2, Menglin Cheng2,
Lu Jiang2, Tiffany R Greenwood2,
Balaji Krishnamachary2, Zaver M Bhujwalla2,
Tone F Bathen1, and Kristine Glunde2,3
1Department of Circulation and Medical
Imaging, Norwegian University of Science and Technology
(NTNU), Trondheim, Norway, 2Department
of Radiology and Radiological Science, Johns Hopkins
University School of Medicine, Baltimore, Maryland,
United States, 3Sidney
Kimmel Comprehensive Cancer Center, Johns Hopkins
University School of Medicine, Baltimore, Maryland,
United States
Here we investigated the effects of targeting choline
phospholipid metabolism using GDPD5 and GDPD6 siRNA in
two breast cancer cell lines, MCF7 and MDA-MB-231. Our
study shows that GDPD5 and GDPD6 siRNA treatment
increases glycerophosphocholine levels, decreases
proliferation and invasion, but did not cause apoptosis.
The effect of GDPD5 siRNA on cell proliferation was more
severe in the less malignant breast cancer cell line.
Decreased cell invasion was observed in GDPD5 compared
to GDPD6 siRNA treated cells. Our results suggest that
GDPD5 and GDPD6 silencing alone/combined can have a
potential role as new molecular targets for treatment of
breast cancer.
|
1115. |
Steady-state susceptibility
contrast MRI detects early anti-angiogenic effects of a
novel biomimetic peptide in a human breast cancer model
Eugene Kim1, Esak Lee1, Charlesa
Plummer2, Stacy Gil1, Alexander S
Popel1, and Arvind P Pathak2
1Department of Biomedical Engineering, Johns
Hopkins University School of Medicine, Baltimore, MD,
United States, 2Department
of Radiology, Johns Hopkins University School of
Medicine, Baltimore, MD, United States
Steady-state susceptibility contrast (SSC)-MRI is a
clinically translatable technique that is used to
measure vascular morphology. We show here that a novel
biomimetic peptide we developed produced strong anti-angiogenic
effects in an orthotopic human breast cancer model. SSC-MRI
was able to detect treatment-induced decreases in blood
volume and vessel caliber before the manifestation of
significant differences in tumor growth and cellularity
(conventional markers of therapeutic efficacy) between
treated and control groups. This suggests that SSC-MRI
provides promising biomarkers of early anti-angiogenic
treatment response that may improve the evaluation and
development of new anti-angiogenic therapies.
|
1116. |
Changes in tumor perfusion
and oxygenation following CA4P administration
Florence Colliez1, Anne-Catherine Fruytier1,
Marie-Aline Neveu1, Julie Magat1,
Bernard Gallez1, and Bénédicte F Jordan1
1Louvain Drug Research Institute, Biomedical
Magnetic Resonance Research Group, University of
Louvain, Brussels, Belgium
Vascular discrupting agents (VDAs) induce tumor hypoxia
within 3 hours in preclinical models. Combretastatin A4
phosphate (CA4P) is the lead compound of this agents’
class. The present work correlates a follow-up on two
tumor models of both tumor oxygenation and tumor
hemodynamics after CA4P administration. Mapping of tumor
oxygenation was assessed with ‘MOBILE’ (Mapping of
Oxygen By Imaging Lipids relaxation Enhancement) a
non-invasive MRI method based on the changes in the
relaxation properties of the tissue lipids protons
whereas tumor hemodynamics (Ktrans and vp) variations
were evaluated by DCE-MRI on same tumor models.
|
1117. |
MRI at 7 T Correlates
Therapy-Induced Alterations in T2 heterogeneity, ADC and
Tumor Volume in Ewing’s Sarcoma Xenografts
Parastou Foroutan1, Christopher L Cubitt2,
Jillaina L Menth3, Damon Reed4,
Olya Grove1, David L Morse1,
Daniel Sullivan5, Robert J Gillies1,
and Gary V Martinez1
1Cancer Imaging & Metabolism, H. Lee Moffitt
Cancer Center & Research Institute, Tampa, FL, United
States, 2Experimental
Therapeutics Program / Translational Research Lab, H.
Lee Moffitt Cancer Center & Research Institute, Tampa,
FL, United States, 3Translational
Research Lab, H. Lee Moffitt Cancer Center & Research
Institute, Tampa, FL, United States, 4Experimental
Therapeutics Program / Sarcoma Program, H. Lee Moffitt
Cancer Center & Research Institute, Tampa, FL, United
States, 5Experimental
Therapeutics Program, H. Lee Moffitt Cancer Center &
Research Institute, Tampa, FL, United States
In spite of the progress with targeted therapies,
response rates for Ewing’s sarcoma (ES), one of the most
aggressive human malignancies, still remains poor. In
addition, imaging approaches assessing therapeutic
response is lacking, as current indices
(volume/diameter) do not accurately correlate with
changes in tumor biology. Herein, profound MRI analyses
were developed to evaluate imaging biomarkers for
Dasatinib and Triciribine treated ES xenografts.
Notably, we showed that inhibited tumor growth was
presaged by elevations in ADC, ADC distribution and T2
heterogeneity. This approach accentuates the role of ADC
as a quantitative imaging biomarker for response and
shows promising clinical relevance in the sarcoma
patient population.
|
1118. |
Non-Invasive Imaging
Biomarkers of Tumor Response to XL184 Therapy
Benjamin A Hoff1, Jean-Christophe Brisset2,
Stefanie Galbán3, Craig J Galbán1,
and Brian D Ross1
1Radiology, University of Michigan, Ann
Arbor, MI, United States, 2New
York University Langone, NY, United States, 3Radiation
Oncology, University of Michigan, MI, United States
Clinical response criteria (RECIST 1.1) considers boney
metastases measuring >10mm without soft tissue
involvement as unmeasurable. The clinical need for
accurate therapeutic response measures is more pressing
with the introduction of targeted therapies into
standard of treatment. XL184 is a novel tyrosine kinase
inhibitor that exhibits activity against mainly MET and
VEGFR-2.1 We evaluated DW-MRI and CT pre- and
post-therapy on a mouse model of bone-metastatic
prostate cancer to assess early treatment response to
this therapy. The therapeutic effect of XL184 was
observed via several readouts, with mean tumor ADC
increasing significantly over controls by day 3
post-therapy.
|
1119. |
Multimodality Imaging
End-Points on mTOR and HSP Inhibition in Pancreatic Cancer:
A Pre-Clinical PET/MRI/MRS Study
Justin Y Lee1, Lora A Wilson2,
Jerri L Choi3, Kendra M Huber4,
Andrea L Merz4, Katerina J Kechris5,
Colin D Weekes2, and Natalie J Serkova4,6
1Department of Anesthesiology, University of
Colorado Anschutz Medical Campus, Aurora, CO, United
States, 2Department
of Oncology, University of Colorado Anschutz Medical
Campus, CO, United States, 3University
of Colorado Anschutz Medical Campus, CO, United States, 4Department
of Anesthesiology, University of Colorado Anschutz
Medical Campus, CO, United States, 5Department
of Biostatics and Informatics, University of Colorado
Anschutz Medical Campus, CO, United States, 6Department
of Radiology, University of Colorado Anschutz Medical
Campus, CO, United States
There is an urgent need to develop novel signal
transduction pathway inhibitor strategies to treat
pancreatic cancer. This project utilizes a combination
of the mTOR inhibitor Everolimus and the HSP-90
inhibitor Ganetepsib with the goal of establishing
metabolic (FDG-PET and 1H-MRS), morphological (DWI), and
anatomical (MRI) end-points to monitor response in mouse
pancreatic adenocarcinoma xenografts. Combination
treatment resulted in decreased tumor growth,
cellularity, and metabolic activity. Our results provide
the first evidence of proliferation and metabolic
response by functional multiparametric imaging and FDG-PET,
DWI and 1H-MRS and identify them as potential biomarkers
in clinical trials.
|
1120. |
Investigating MRI
Biomarkers as Indicators of Early Treatment Response in a
Triple Negative Model of Breast Cancer
Stephanie L. Barnes1,2, Jennifer G. Whisenant1,2,
J. Oliver McIntyre1,3, and Thomas E.
Yankeelov1,2
1Vanderbilt University Institute of Imaging
Sciences, Vanderbilt University, Nashville, TN, United
States, 2Radiology
and Radiological Sciences, Vanderbilt University,
Nashville, TN, United States, 3Cancer
Biology, Vanderbilt University, Nashville, TN, United
States
This work aims to assess the feasibility of diffusion
weighted and dynamic contrast enhanced MRI (DW- and DCE-MRI,
respectively) parameters as early (i.e., before tumor
volume changes) indicators of treatment response to
Abraxane in a preclinical model of triple negative
breast cancer. We found that ADC and Ktrans were
significantly different from the control group in both
high and low dose treatment groups on day 2, prior to
any observable difference in the tumor size. These
results indicate that ADC from DW-MRI and Ktrans from
DCE-MRI could serve as noninvasive, early indicators of
treatment response.
|
1121. |
Evaluation of tumor
oxygenation in response to an indole-based vascular
disrupting agent using 19F
MRI
Heling Zhou1, Rami R Hallac2,
Rebecca Denney1, Li Li1, Ramona
Lopez1, Li Liu1, Edward E Graves3,
Mary Lynn Trawick4, Kevin G Pinney4,
and Ralph P Mason1
1Radiology, University of Texas Southwestern
Medical Center, Dallas, TX, United States, 2Analytical
Imaging and Modeling Center, Children's Medical Center,
Dallas, TX, United States, 3Radiation
Oncology and Radiology, Stanford University, CA, United
States, 4Chemistry
and Biochemistry, Baylor University, Waco, TX, United
States
Oxi8007, a novel vascular disrupting agent, showed rapid
and highly selective shutdown of tumor vasculature. In
this study we explored the onset of hypoxia with FREDOM,
a 19F
oxygen mapping technique, to assess the pO2 changes
following the administration of Oxi8007 at two different
doses using an orthotopic breast cancer mouse model.
Both dose groups showed rapid decrease of pO2 though
with a slower rate accompanying the lower dose. PO2 maps
revealed heterogeneous responses to the drug.
|
1122. |
Assessment of tumor
physiological changes following hypo-fractionated SBRT using
multi-parametric MRI
Heling Zhou1, Rebecca Denney1,
Zhang Zhang2, Debabrata Saha2, and
Ralph P Mason1
1Radiology, University of Texas Southwestern
Medical Center, Dallas, TX, United States, 2Radiation
Oncology, University of Texas Southwestern Medical
Center, Dallas, TX, United States
Tumor hypoxia is an important biomarker related to tumor
treatment response, but non-invasive measurements in
vivo require further development, application and
validation. We have applied oxygen enhanced MRI together
with DCE MRI to explore the longitudinal effects of
hypofractionated stereotactic body radiation therapy on
tumor re-oxygenation and development. BOLD and TOLD
responses to oxygen breathing challenge were found to
decrease following radiation. Quantitative T2*
also showed the same trend, whereas quantitative DCE
parameters (ve and
Ktrans) remained unchanged. These
observations suggest potential noninvasive assessment of
tumor re-oxygenation for treatment planning.
|
1123. |
A role for DCE MRI in
predicting tumor radiation response
Rami Hallac1,2, Heling Zhou1,
Rajesh Pidikiti3,4, Kwang Song3,5,
Strahinja Stojadinovic3, Dawen Zhao1,
Vikram Kodibagkar1,6, Peter Peschke7,
Timothy Solberg3,8, and Ralph Peter Mason1
1Radiology, UT Southwestern, Dallas, TX,
United States, 2Children's
Medical Center, Dallas, TX, United States, 3Radiation
Oncology, UT Southwestern, Dallas, TX, United States, 4MD
Anderson, TX, United States, 5Henry
Ford Hospital, MI, United States, 6Biological
and Health Systems Engineering, Arizona State
University, Tempe, AZ, United States, 7German
Cancer Center, Heidelberg, D-69120, Germany, 8Univ
Pennsylvania, PA, United States
DCE MRI has been extensively studied and suggested to be
a useful method for evaluating tumor hypoxia. Here, we
evaluated correlations between quantitative DCE MRI and
radiation outcome of the well characterized syngeneic
Dunning prostate rat tumor R3327-AT1. Following DCE MRI,
8 tumors were irradiated with a single dose of 30 Gy,
while rats breathed air or oxygen, whereas two served as
non-irradiated controls. Irradiation caused significant
tumor growth delay. Strong correlation was observed
between tumor growth delay and ve, but there no obvious
correlation with Ktrans. High temporal resolution DCE
MRI could provide predictive insight into response to
radiation.
|
1124. |
Monitoring response to
drug-loaded PLGA nanoparticles in a Mia PaCa-2 pancreatic
tumor model with T2 and diffusion-weighted MRI
Joseph E Kobes1, Iman Daryaei2,
Christine M Howison1, Emmaneulle J. Meuillet3,
and Mark Pagel4,5
1Biomedical Engineering, University of
Arizona, Tucson, Arizona, United States, 2Chemistry
and Biochemistry, University of Arizona, Tucson, AZ,
United States, 3University
of Arizona Cancer Center, University of Arizona, Tucson,
Arizona, United States, 4Dept.
of Biomedical Engineering, University of Arizona,
Tucson, Arizona, United States,5Dept. of
Chemistry and Biochemistry, University of Arizona,
Tucson, Arizona, United States
Poly(lactic-co-glycolic) acid nanoparticles (PLGA-NP)
can improve delivery of PHT-427, a promising
AKT-inhibitory chemotherapeutic against pancreatic
cancer. To assess the improved therapeutic effect of
PLGA-NP-loaded with PHT-427 (PLGA-PH-427), this study
employed parametric maps of the Apparent Diffusion
Coefficient (ADC) and T2 relaxation time to localized
orthotopic pancreatic tumors, and employed ADC
measurements to track tumor response to therapy,
following treatment of a MiaPaCa-2 pancreatic tumor
model with PHT-427 or PLGA-PHT-427.
|
1125. |
MRI guided drug delivery
targeting glioma using inteleukin-13 conjugated liposome
(IL-13-Liposome)
Xiaoli Liu1, Achuthamangalam Madhankumar1,
Patti Miller2, Becky Webb1, Susan
Hafenstein3, Elias Rizk1, James
Connor1, and Qing Yang4
1Neurosurgery, Pennsylvania State College of
Medicine, Hershey, PA, United States, 2Radiology,
Pennsylvania State College of Medicine, Hershey, PA,
United States,3Medicine, Pennsylvania State
College of Medicine, Hershey, PA, United States, 4Pennsylvania
State College of Medicine, Hershey, PA, United States
There is a critical need for MRI guided drug delivery
for treating glioma. We developed a liposome
specifically targeting glioma using interlukin-12
receptors as the target for the tumor cells
(IL-13-Liposome). Our in vivo and in vitro data
demonstrated that our targeted liposome is capable of
delivering anticancer drug and MRI contrast agent to the
tumor cells at the same time.
|
1126. |
Pharmacokinetic modelling
of longitudinal dceMRI scans for assessment of tumour growth
Monica Enescu1, Amalia Cifor1,
Veerle Kersemans2, Danny Allen2,
Stuart Gilchrist2, John Beech2,
Sean Smart2, Michael A Chappell1,
and Julia A Schnabel1
1Institute of Biomedical Engineering,
University of Oxford, Oxford, United Kingdom, 2Preclinical
Imaging Group, University of Oxford, Oxford, United
Kingdom
A new model based approach to quantify tumour growth
from longitudinal dceMRI images is proposed. Subsequent
time points were registered to the first time point
using a multichannel registration method based on
pharmacokinetic parameter maps. This method was shown to
successfully recover tumour growth, on data where the
tumour change is small and gradual. We have also
investigated whether pharmacokinetic parameters at the
first time point can act as a predictor of localized
tumour growth.
|
1127. |
Towards MRI-based
measurement of tissue oxygen content
Scott C. Beeman1, John A. Engelbach1,
Joseph J.H. Ackerman1,2, and Joel R. Garbow1
1Department of Radiology, Washington
University in Saint Louis, Saint Louis, Missouri, United
States, 2Department
of Chemistry, Washington University in Saint Louis,
Saint Louis, Missouri, United States
We, and others, are pursuing a technique to measure
tissue oxygenation that takes advantage of the
paramagnetic property of molecular oxygen, as found
dissolved in tissue. Herein, we present a R1-based
breathing gas challenge technique that can distinguish
radiation damage from tumor - a distinction which has
been difficult to make using other methods. We further
show that the R1 of
brain parenchyma can be measured by isolating the R1 of
bulk water and suppressing flow contributions, and that
breathing of carbogen gas has a direct impact on the R1 of
brain parenchyma.
|
1128. |
Monitoring tumor response
to the direct or indirect targeting of choline
Lionel Mignion1, Pierre Danhier1,
Paolo E. Porporato2, Julie Magat1,
Pierre Sonveaux2, Vincent Gregoire3,
Bernard Gallez1, and Benedicte F. Jordan1
1Biomedical Magnetic Resonance Unit, Louvain
Drug Research Institute, Université Catholique de
Louvain, Brussels, Belgium, 2Pole
of pharmacology, Institut de Recherche Expérimentale et
Clinique, Université Catholique de Louvain, Brussels,
Belgium, 3Pole
of Molecular Imaging, Radiotherapy and Oncology,
Université Catholique de Louvain, Brussels, Belgium
The aim of the current study is to assess response to
the modulation of the choline pathway, that is known to
be involved in oncogenesis, by using specific choline
kinase and transporters inhibitors and shRNA of choline
kinase. In this work we proposed a combination of
choline spectroscopy and diffusion markers to predict
the tumor evolution after treatment. Using these
combined markers we can assess the actual inhibition of
the target in vivo and assess early tumor response non
invasively, in order to avoid drug resistance with the
ultimate goal of improving therapy individualization.
|
1129. |
Toward Distinguishing
Radiation Effects from Tumor Regrowth in an Irradiated
Glioma Model
Carlos J Perez-Torres1, John A Engelbach1,
Jeremy Cates2, Dinesh K Thotala2,
Robert E Drzymala2, Joseph JH Ackerman1,3,
and Joel R Garbow1
1Department of Radiology, Washington
University, Saint Louis, MO, United States, 2Department
of Radiation Oncology, Washington University, Saint
Louis, MO, United States, 3Department
of Chemistry, Washington University, Saint Louis, MO,
United States
A major unmet challenge in the treatment of brain tumors
is non-invasively differentiating recurrent tumor from
delayed radiation injury. Our work focused on the
difference in cellularity between tumor and radiation
injury via Diffusion Weighted Imaging (DWI) and
Magnetization Transfer Contrast (MTC) MRI. Our results
in preclinical rodent models suggest that DWI may help
discriminate between tumor and radiation effects while
MTC, though sensitive , is mostly incapable of
differentiating between tumor and radiation effects.
|
1130. |
Adaptive Therapy: A Novel
Cancer Treatment Regimen Using MRI.
Pedro M Enriquez-Navas1, Tuhin Das1,
Yoonseok Kam1, Parastou Foruotan1,
Gary Martinez1, Robert J Gillies1,
and Robert A Gatenby2
1Cancer Imaging and Metabolism, Moffitt
Cancer Center, Tampa, Florida, United States, 2Radiology,
Moffitt Cancer Center, Tampa, Florida, United States
Cancer is treated with the highest possible dose of
drug, depending on toxicity, to achieve the maximum drug
effect. However, this is a flawed approach because of
the evolutionary dynamics that depend on the variable
fitness across the tumor. Thus, the treatment scheduling
is suboptimal. Adaptive therapy (AT) is a novel cancer
therapy. The dose is dependent on the tumor status. The
key point is that AT has been demonstrated to promote
the growth of chemosensitive tumor cells at the expense
of chemoresistant ones. With the focus on translation,
we are applying MRI tools to fine tune AT in vivo.
|
1131. |
pH-sensitive nanoparticle
for delivery of lonidamine to triple-negative breast cancer:
A preliminary 31P MRS study
Kavindra Nath1, Hoon Choi1, David
S Nelson1, Daniel F Heitjan1,
Dennis B Leeper2, Jerry D Glickson1,
I-Wei Chen1, and Rong Zhou1
1University of Pennsylvania, Philadelphia,
Pennsylvania, United States, 2Thomas
Jefferson University, Philadelphia, Pennsylvania, United
States
To exploit the slightly acidic extracellular pH
environment of cancer in comparison with normal tissue,
we have made ultra pH-responsive peptide nanoparticles
to encapsulate lonidamine (LND), an antineoplastic
agent, for intravenous administration. Once at tumor
site (pHe = 6.9), the nanoparticles melt, releasing LND
molecules that diffuse to surrounding cancer cells. In
normal tissues (pHe ≥ 7.2), however, LND will not be
released as the nanoparticles remain stable. Our results
show that pH-responsive nanoparticles efficiently
solubilize LND for i.v. injections and substantially
increase the tumor bioavailability of LND.
|
1132. |
Chemotherapy resistant,
dormant Glioblastoma cells exhibit high rates of oxidative
metabolism
Tomoyuki Mashimo1, Kumar Pichumani2,
Koji Sagiyama2, Vamsidhara Vemireddy1,
Shyam Sirasanagandla1, Suraj Nannepaga1,
Kimmo Hatanpaa3, Masaya Takahashi2,
Ralph DeBeraridinis4, Elizabeth Maher1,
Craig Malloy2, and Robert Bachoo1
1Neurology and Neurotherapeutics, UT
Southwestern Medical Center, Dallas, TX, United States, 2Advanced
Imaging Research Center, UT Southwestern Medical Center,
Dallas, TX, United States, 3Pathology,
UT Southwestern Medical Center, Dallas, TX, United
States, 4Children's
Medical Center Research Institute, UT Southwestern
Medical Center, Dallas, TX, United States
Chemotherapy resistant brain tumor (GBM) cells posses
high rates oxidative metabolism
|
1133. |
Gallium maltolate inhibits
angiogenesis in brain tumor xenograft model
Kimberly R Pechman1, Andrew Lozen1,
Christopher R Chitambar2, and Kathleen M
Schmainda3
1Neurosurgery, Medical College of Wisconsin,
Milwaukee, WI, United States, 2Medicine,
Medical College of Wisconsin, Milwaukee, WI, United
States, 3Radiology
& Biophysics, Medical College of Wisconsin, Milwaukee,
WI, United States
Malignant brain tumors are difficult to treat and
patient survival is dismal. MRI measures of enhancing
tumor volume have proven unreliable since decreases in
enhancement may be independent of biologic effect. The
purpose of this study was to investigate a novel
therapy, gallium maltolate, for brain tumors using the
U87 xenograft model. In this study we used steady state
and DSC-MRI to measure tumor blood volume and flow. The
studies, demonstrate that the novel gallium maltolate
therapy inhibits brain tumor angiogenesis.
|
1134. |
Feasibility of MR-guided
needle-directed intratumoral HoMS delivery for localized
radiation therapy in a large tumor-model
Bo Sybren van Leeuwen1, Sebastiaan Alexander
van Nimwegen2, Frank Zijlstra3,
Chris Oerlemans3, Jolle Kirpensteijn2,
Johannes Franciscus Nijsen4, and Peter Roland
Seevinck3
1Dept. of Clinical Sciences of Companion
Animals, Faculty of Veterinary Medicine Utrecht
University, Utrecht, Utrecht, Netherlands, 2Dept.
of Clinical Sciences of Companion Animals, Faculty of
Veterinary Medicine Utrecht University, Utrecht,
Netherlands, 3Image
Sciences Institute, Imaging Division, University Medical
Center Utrecht, Utrecht, Utrecht, Netherlands, 4Imaging
Division, University Medical Center Utrecht, Utrecht,
Netherlands
In this study, we demonstrated the feasibility of MR-guided
needle-directed intratumoral 165HoMS delivery in a large
tumor model. MRI facilitated tumor visualization, entry
point determination and needle trajectory planning. The
presented approach enabled dynamic monitoring of the
needle insertion and needle tip positioning in the
tumor, allowing intraprocedural optimization of HoMS
delivery. coRASOR reconstruction was demonstrated to
improve needle visualization by generating positive
contrast, causing the titanium needles to be easily
identified with high spatial and temporal resolution
when applied prospectively. Future work should also aim
at facilitating intraprocedural dosimetry to enable
optimization of the number of injection sites and the
amount of HoMS to be delivered to eventually provide a
favorable dose distribution on the tumor, while sparing
the healthy tissue.
|
1135. |
Nitroxoline induces
apoptosis and slows glioma growth in vivo
Jelena Lazovic1, Lea Guo1,
Jonathan Nakashima2, and Whitney Pope3
1Radiology, University of California, Los
Angeles, California, United States, 2Molecular
and Medical Pharmacology, University of California, Los
Angeles, California, United States, 3University
of California, Los Angeles, California, United States
Chemotherapeutic potential of FDA approved small
molecule nitroxoline was evaluated in preclinical
Pten/Kras glioma mouse model. The glioma volume before
and after nitroxoline therapy was measured using
T2-weighted MR images. Apparent diffusion coefficient
and T2-values were quantified in order to determine if
they can be used to predict treatment response. A
significant reduction in glioma growth at 7 and 14 days
was accompanied with significant increase in ADC values,
while there was no change in T2-values. Histological
examination and TUNEL staining revealed significantly
more TUNEL-labeled cells in nitroxoline treated mice,
implicating nitroxoline is potent at inducing apoptosis
in this model.
|
1136. |
Selective acidification and
de-energization of A2780 ovarian cancer xenografts using
lonidamine: A preliminary 1H and 31P MRS study
Kavindra Nath1, Ting Liu1, David S
Nelson1, Daniel F Heitjan1, Dennis
B Leeper2, Jerry D Glickson1,
I-Wei Chen1, and Rong Zhou1
1University of Pennsylvania, Philadelphia,
Pennsylvania, United States, 2Thomas
Jefferson University, Philadelphia, Pennsylvania, United
States
In vivo 31P Magnetic Resonance Spectroscopy demonstrates
that A2780 ovarian cancer xenografts treated with the
monocarboxylate transporter-1 (MCT-1) inhibitor,
lonidamine (LND), exhibits a sustained and
tumor-selective decrease in delta pHi and pHe of 0.56 ±
0.10 (p < 0.05) and 0.34 ± 0.23 (p = 0.05) respectively.
Tumor bioenergetics (βNTP/Pi) decreased by 70.0 ± 22% (p
< 0.05) and integrated intensities of the steady-state
tumor lactate were increased after 40 min. (p < 0.05)
relative to the baseline level following LND
administration. The decline of pHi and bioenergetics
could be critical parameters for chemo- and
thermo-sensitization of ovarian cancers.
|
1137. |
Serial Imaging of
Physiological and Metabolic Changes in Response to
Radiotherapy with Tumor-Bearing Mice
Masayuki Matsuo1, Shingo Matsumoto1,
Keita Saito1, Yoichi Takakusagi1,
Douglas Morris2, Jeeva Munasinghe2,
Nallathamby Devasahayam1, Sankaran
Subramanian1, James Mitchell1, and
Murali Krishna1
1Radiation Biology Branch, National Institues
oh Health, North Bethesda, MaryLand, United States, 2National
Institute of Neurological Disorder and Stroke, National
Institues oh Health, North Bethesda, MaryLand, United
States
A non-invasive co-imaging system of pO2 and pyruvate
metabolism was developed to visualize the correlation
between tumor oxygen status and energy metabolism.
SCCVII and HT29 were compared when the size of both
tumors was similar. We investigated the effect of single
5 Gy irradiation on the relationship in HT29 tumors.
SCCVII has significantly larger hypoxic sub-region (pO2
< 8 mmHg) than HT29. Lactate/pyruvate ratio in 0-8mmHg
of 1 day after 5Gy irradiation of HT29 is higher than of
non irradiation of HT29 that is explained by decreased
perfusion, decreased tumor pO2, and increased
extracellular acidification rate.
|
1138. |
Dynamic MRS of
hyperpolarized 1-13C pyruvate in brain tumor
afflicted mice treated with temozolomide
Teresa Delgado-Goñi1,2, Eva Monteagudo3,
Miquel E. Cabañas3, Carles Arús1,2,
and Silvia Lope-Piedrafita3
1Department de Bioquímica i Biologia
Molecular, Unitat de Bioquímica de Biociències,
Universitat Autònoma de Barcelona, Cerdanyola del Vallès,
Barcelona, Spain, 2Centro
de Investigación Biomédica en Red en Bioingeniería,
Biomateriales y Nanomedicina (CIBER-BBN), Cerdanyola del
Vallès, Barcelona, Spain, 3Servei
de RMN, Universitat Autònoma de Barcelona, Cerdanyola
del Vallès, Barcelona, Spain
In this study we aimed to evaluate the detection of
response to temozolomide therapy in a well characterized
mouse brain glioma model by hyperpolarized [1-13C]
pyruvate. Quantification of time course 13C spectra
showed significant differences between wildtype and
untreated-glioblastoma-bearing mice in the lactate
signals from 12s to 50s post-injection. However no
differences were observed in lactate between untreated
and treated glioblastoma-bearing mice. Nevertheless,
individual Lac/Pyr ratios of treated mice seemed to have
two separate patterns, one with increased ratios and the
other with smaller values, which could indicate
different behavior with respect to therapy response
variability in the evaluated mice.
|
1139. |
Preliminary evidence of a
vascular normalization biomarker in trastuzumab-treated
HER2+ breast cancer
Anna G. Sorace1,2, Jennifer G. Whisenant1,2,
J. Oliver McIntyre2,3, Violeta M. Sanchez4,
Mary E. Loveless2, and Thomas E. Yankeelov1,2
1Radiology, Vanderbilt University, Nashville,
Tennessee, United States, 2Vanderbilt
University Institute of Imaging Science, Vanderbilt
University, Nashville, Tennessee, United States, 3Cancer
Biology, Vanderbilt University, Nashville, Tennessee,
United States, 4Hematology
Oncology, Vanderbilt University, Nashville, Tennessee,
United States
We use quantitative DCE-MRI to determine sensitivity to
HER2+ targeted breast cancer treatments early in the
course of therapy. Preclinical studies utilizing mice
with HER2+ (sensitive or resistant) tumors were treated
with trastuzumab or saline. DCE-MRI was longitudinally
tracked from baseline to day 4. DCE-MRI parameter, Ktrans,
revealed significant increases post treatment in the
HER2+ sensitive, treated tumors compared to their
control counterparts, untreated and HER2+ resistant
treated, therefore suggesting vessel normalization.
Paralleled histological parameter, microvessel density,
also revealed significant increases. Imaging biomarkers
have potential as a noninvasive tool to discriminate
responders from nonresponders early during the course of
therapy.
|
1140. |
Lonidamine sensitizes human
breast cancer xenografts to Doxorubicin via metabolic
modulations
Kavindra Nath1, Jerry D Glickson1,
David S Nelson1, Daniel F Heitjan1,
Dennis B Leeper2, I-Wei Chen1, and
Rong Zhou1
1University of Pennsylvania, Philadelphia,
Pennsylvania, United States, 2Thomas
Jefferson University, Philadelphia, Pennsylvania, United
States
We demonstrate that a small molecule, lonidamine (LND),
sensitizes breast cancers to the chemotherapeutic drug,
Doxorubicin, via selective intracellular acidification
and suppression of high energy phosphate production of
the tumor. In vivo MR spectroscopy of human breast
cancer xenografts show that LND treatment induces a
maximal decrease of intracellular pH of 0.54 unit and
depletion of NTP/Pi by 77% accompanied by 3-fold
increase of tumor lactate content. One treatment with
LND (100 mg/kg, i.p.) combined with one injection of
doxorubicin (12 mg/kg, i.v.) leads to a tumor growth
delay of 23 days and log10 cell-kill of 1.70. These
results suggest that LND potentiates chemotherapeutics
by modulating cancer metabolism.
|
|
|
TRADITIONAL
POSTER SESSION ○ CANCER |
Cancer Preclinical Animal Studies
Monday 12 May 2014
Traditional Poster Hall |
10:45 - 12:45 |
|
|
1141. |
Dynamic 3D Compressed
Sensing MR of hyperpolarized 13C Pyruvate and Urea in
Prostate Cancer Models
Hsin-Yu Chen1, Peder E. Z. Larson2,
Cornelius von Morze2, Christine Leon Swisher1,
Naeim Bahrami2, Robert Bok2, John
Kurhanewicz1,2, and Daniel B. Vigneron1,2
1Graduate Program in Bioengineering, UCSF and
UC Berkeley, San Francisco, California, United States, 2Department
of Radiology and Biomedical Imaging, University of
California, San Francisco, California, United States
Use of 3D compressed-sensing [13C]pyruvate and [13C]urea
MRSI sequence and dynamic models enables, for the first
time, simultaneous evaluation of metabolic and perfusion
parameters kpl and ktrans in a preclinical prostate
tumor model. We demonstrates increases in both pyruvate-to-lactate
conversion rate and perfusion/permeability in prostate
tumor versus normal tissue. This approach shows great
potential for the quantitative assessment of prostate
cancer aggressiveness and also treatment response.
|
1142. |
Simultaneous Hyperpolarized
13C Pyruvate and Urea Perfusion Parameterizations in Cancer
Naeim Bahrami1, Cornelius Von Morze1,
Christine Leon1, Daniel B. Vigneron1,
and Peder E.Z. Larson1
1Department of Radiology and Biomedical
Imaging, University of California, San Francisco,
California, United States
In cancerous tissue there is both existing vasculature
and neovascularization as different kinds of lesions
surpass the normal blood supply, including small
circulation disturbance in some of the abnormal vessels.
The variation of pyruvate perfusion and urea perfusion
can be observed for the healthy and cancerous tissues.
The urea perfusion is primarily representing the
vasculature delivery in each specific tissue and it
stays in the vessels, while the pyruvate perfusion,which
is the accumulation of all source and derived
metabolites related to the pyruvate including
pyruvate,lactate and alanine, can also be a marker for
vascular delivery but also includes tissue uptake.
|
1143. |
19F MRI of
Colitis-Associated Colon Cancer (CACC) in a Murine Model of
Inflammatory Bowel Disease
Deepak K. Kadayakkara1,2, Soo Hyun Shin3,4,
and Jeff W. M. Bulte2,3
1Dept. of Oncology, The Johns Hopkins School
of Medicine, Baltimore, Maryland, United States, 2Dept.
of Radiology and Radiological Science, The Johns Hopkins
School of Medicine, Baltimore, Maryland, United States, 3Cellular
Imaging Section, Institute for Cell Engineering, The
Johns Hopkins School of Medicine, Baltimore, Maryland,
United States, 4Dept.
of Biomedical Engineering, The Johns Hopkins School of
Medicine, Baltimore, Maryland, United States
Invasive colonoscopy has showed that the severity of
colon inflammation correlates with the development of
colitis-associated colon cancer (CACC). We applied 19F
MRI to non-invasively image inflammation and
premalignant tumor formation. Mice were treated with
azoxymethane and dextran sodium sulfate to induce CACC.
The course of inflammation and tumor development was
determined with MRI following injection of
perfluorocarbons that are taken up by macrophages. 19F
signals were detected from the colon wall, with tumors
arising from the same anatomical sites. Thus, 19F MRI
appears useful to further characterize the relationship
between bowel inflammation and risk of CACC.
|
1144. |
Combined Magnetic Resonance
Spectroscopy and Mass Spectrometry Imaging of Breast Tumor
Hypoxia
Asif Rizwan1, Lu Jiang1, Nadine
Mascini2, Vadappuram P Chacko1,
Menglin Cheng1, Venu Raman1,3,
Zaver M Bhujwalla1,3, Ron Heeren2,
and Kristine Glunde1,3
1Radiology and Radiological Science, The
Johns Hopkins University School of Medicine, Baltimore,
Maryland, United States, 2FOM
Institute AMOLF, Amsterdam, Netherlands,3The
Sidney Kimmel Comprehensive Cancer Center, The Johns
Hopkins University School of Medicine, Baltimore,
Maryland, United States
Our goal is to identify a probe for imaging hypoxia in
breast cancer models, which can be detected in vivo by
magnetic resonance spectroscopy (MRS) and ex vivo by
mass spectrometry imaging (MSI). We tested hypoxyprobe
F6, which was intravenously injected in breast tumor
xenograft bearing mice, and detected in vivo using 19F
MRS. Following sacrifice of mice and tumor removal, the
hypoxia probes F6 and pimonidazole were imaged for the
first time ex vivo by matrix-assisted laser desorption
ionization (MALDI) MSI. Hypoxyprobe F6 has the potential
to be a multimodality imaging reporter for hypoxia
detection by MRS and MSI.
|
1145. |
Neurochemical profile
differentiation of glioma induced by cancer stem cells
expressing WIF1: a 1H-MRS
longitudinal study at 14.1T
Marta Lai1, Cristina Cudalbu2,
Bernard Lanz1,3, Irene Vassallo4,
Marie-France Hamou4, Monika Hegi4,
and Rolf Gruetter2,5
1Laboratory of Functional and Metabolic
Imaging (LIFMET), Ecole Polytechnique Fédérale de
Lausanne, Lausanne, Switzerland, 2Centre
d’Imagerie Biomedicale, Ecole Polytechnique Fédérale de
Lausanne, Lausanne, Switzerland, 3Department
of Radiology, University of Lausanne, Lausanne,
Switzerland, 4Laboratory
of Brain Tumor Biology and Genetics, Department of
Neurosurgery, Lausanne University Hospital, Lausanne,
Switzerland, 5Departments
of Radiology, University of Lausanne and Geneva,
Switzerland
WIF1 gene has been recently identified as a tumor
suppressor gene in glioblastoma. Human glioma stem cells
have been genetically modified for the expression of the
WIF1 gene, they were injected intracranially in NUDE
mice for 1H
MRS analysis and compared with a group of mice injected
with the analogue cell line without modifications.
Quantification of 1H
MRS spectra acquired longitudinally throughout the tumor
development showed distinct metabolic features in the
two groups of mice which correlate with a less
aggressive phenotype for glioma stem cells expressing
WIF1.
|
1146. |
Localized, Non-invasive In
Vivo Measurement of Enzymatic Activity using MAD-STEAM HP
13C MRSI
Christine Leon Swisher1,2, Peder E.Z. Larson1,2,
Robert A. Bok1, Justin Delos Santos1,
Romelyn Delos Santos1, Hsin-Yu Chen1,2,
Adam B. Kerr3, John M. Pauly3,
Sarah J. Nelson1,2, John Kurhanewicz1,2,
and Daniel B. Vigneron1,2
1Department of Radiology and Biomedical
Imaging, University of California, San Francisco, San
Francisco, CA, United States, 2UC
Berkeley-UCSF Graduate Program in Bioengineering, San
Francisco, CA, United States, 3Magnetic
Resonance Systems Research Laboratory, Department of
Electrical Engineering, Stanford University, Stanford,
CA, United States
MAD-STEAM MRSI provides a simple and robust method for
parametric mapping with increased specificity to
cellular exchange without concomitant signals from
arterial input or T1 relaxation. We show that this
technique correlates with enzymatic activity (R2= 0.883)
and can be used to non-invasively measure enzymatic
activity in vivo and identify regions with high
enzymatic activity (p-value = 0.003). In the field of
oncology in particular, this new technique has great
biomedical and clinical significance, as it could be
used to better identify particularly aggressive regions
within tumors, target image-guided biopsies, monitor
cancer progression, and follow response to therapy.
|
1147. |
Effect of c-Myc Expression
on Cellular-Interstitial Water Exchange Kinetics:
Conditional Transgenic Mouse Breast Cancer Model
Ramesh Paudyal1, Sergey Magnitsky2,
Steve Pickup3, Lewis A. Chodosh4,
Charles Springer5, and Jerry D. Glickson3
1Yerkes Imaging Center, Yerkes Regional
Primate Research Center, Emory University, Atlanta, GA,
United States, 2Radiology,
USCF, CA, United States, 3Radiology,
University of Pennsylvania, Philadelphia, PA, United
States, 4Department
of Cancer Biology, University of Pennsylvania,
Philadelphia, PA, United States, 5Advanced
Imaging Research Center, Oregon Health & Science
University, OR, United States
In this study, we evaluate the effect on
cellular-interstitial water exchange in Transgenic
MTB/TOM mice DCE-MRI data, which conditionally express
the human oncogene c-myc in mammary glands in response
to doxycycline (dox) treatment, using Shutter Speed
Model (SSM). The data were measured with dox and 4 days
after withdrawal of dox. Herein, we observed a
significant decrease in Ktrans and ti after a removal of
dox. Changes in Ktrans and ti might serve as surrogate
biomarkers in breast cancer study.
|
1148. |
Correlation between in
vivo and ex
vivo MRI of
mouse mammary glands with regards to apparent diffusion
coefficient and T2 values
Xiaobing Fan1, Kay Macleod2,
Devkumar Mustafi1, Suzanne D Conzen3,
Erica Markiewicz1, Marta Zamora1,
Jim Vosicky1, Jeffrey Mueller4,
and Gregory S Karczmar1
1Department of Radiology, The University of
Chicago, Chicago, IL, United States, 2Ben
May Department for Cancer Research, The University of
Chicago, Chicago, IL, United States, 3Medicine,
Hematology/Oncology, The University of Chicago, Chicago,
Chicago, IL, United States, 4Department
of Pathology, The University of Chicago, Chicago, IL,
United States
High resolution ex vivo imaging can improve
understanding of cancer and guide evaluation of surgical
specimens. The rationale for ex vivo MRI is strengthened
if there is a strong correlation between ex vivo and in
vivo images. Here we evaluate MRI at 9.4 Tesla of a
mouse model (n = 7) of breast cancer. For ex vivo
experiments, excised skin and glands were wrapped around
a sponge to maintain the in vivo spatial configuration.
There was a strong correlation (0.73 < r < 0.86, p <
0.0001) between the in vivo and ex vivo ADC’s and T2’s.
|
1149. |
Dual biomarker CEST-MRI
evaluates tumor pH and vascular perfusion in an orthotopic
ovarian cancer model
Liu Qi Chen1, Kyle Mitchell Jones2,
Christine Howison3, Setsuko K Chambers4,
Amanda Baker5, and Mark Pagel6
1Chemistry, University of Arizona, Tucson,
Arizona, United States, 2Biomedical
Engineering, University of Arizona, Tucson, AZ, United
States, 3Biomedical
Engineering, University of Arizona, Tucson, Arizona,
United States, 4Obstetrics
and gynecology, University of Arizona, Arizona, United
States, 5Pharmacology,
University of Arizona, Tucson, Arizona, United States, 6Biomedical
Engineering and Chemistry, University of Arizona,
Tucson, Arizona, United States
Extracellular pH (pHe) is a hallmark for tumor
microenvironment. AcidoCEST MRI is a noninvasive MRI
method that can measure pHe to assess tumor acidosis.
This method allows for a pixel by pixel pH analysis that
can accurately determine spatial heterogeneity of the
tumor as well as contrast agent uptake. In this study,
acidoCEST MRI was used to assess an SKOV3 ovarian tumor
model. Our results showed that the tumor model was
mildly acidic, with an average pH of 6.88. Additionally,
tumor acidosis and lower perfusion were correlated with
larger ovarian tumors.
|
1150. |
Feasibility of amide proton
transfer imaging of rodent glioblastoma model at 3T clinical
scanner
Jinsuh Kim1 and
Phillip Zhe Sun2
1Radiology, University of Iowa, Iowa City,
IA, United States, 2Radiology,
A. A. Martinos Center for Biomedical Imaging,
Massachusetts General Hospital, Boston, MA, United
States
In this work, a practical amide proton transfer (APT)
imaging method for small animal brain at 3T clinical
scanner was developed using a multi-shot sequence with
k-space trajectory of 2D interleaved variable-density
(VD) spiral-out. This method was applied on 4
orthotropic GBM xenograft models in immune-deficient
rats. This study demonstrated elevated APT effect within
the tumors with measured APT ratio ranging from 3.40 to
5.28% (4.2±0.83; mean±S.D.) consistent with prior
studies. Efficient use of gradient hardware in VD spiral
sequence allowed small field-of-view acquisition while
maintaining reasonable signal-to-noise ratio for small
animal brain scan at clinical 3T scanner.
|
1151. |
Redox state imaging in a
mouse model of aggressive prostate cancer
Alan B McMillan1, Bilal Bin-Hafeez2,
Ajit K Verma2, Weixiong Zhong3,
Terry D Oberley3, and Luksana Chaiswing3
1Radiology, University of Wisconsin, Madison,
Wisconsin, United States, 2Human
Oncology, University of Wisconsin, Madison, Wisconsin,
United States, 3Pathology
and Laboratory Medicine, University of Wisconsin,
Madison, Wisconsin, United States
The use of stable free radical contrast agents
(nitroxides) has been demonstrated in MRI and electron
paramagnetic resonance imaging (EPRI). The agent
4-Hydroxy-2,2,6,6-tetramethylpiperidine-N-oxyl (TEMPOL)
is a superoxide dismutase mimetic that also shortens
longitudinal relaxation time (T1). After intravenous
administration, the temporal rate of T1-weighted signal
normalization is increased in tissues that are more
oxidizing. The redox status (balance of oxidizing and
reducing species) is important in cancer progression,
where cancer aggressiveness is related to increased
tissue oxidation. The purpose of this work is to
investigate the feasibility of measuring TEMPOL signal
dynamics in mouse models of prostate cancer.
|
1152. |
Direct imaging of tumor
cellularity using restriction spectrum imaging in a
xenograft mouse GBM model
Tuva Hope1,2, Joshua Kuperman3,
Anders Dale3, and Nate White3
1Medical Imaging Lab, NTNU, Trondheim,
Trondheim, Norway, 2Intervention
Center, Oslo University Hospital, Oslo, Oslo, Norway, 3Multimodal
Imaging Lab - UCSD, San Diego, United States
Using a GBM xenograft mouse model we demonstrate how
restricted water signal, as measured with constant
b-value, multi diffusion time diffusion experiment,
provides a novel contrast mechanism for identifying
cancer cells in vivo.
|
1153. |
1 Tesla Bench-top MRI of a
Mouse Model of Colorectal Carcinoma Metastasis in the Liver:
Comparison with 9.4 Tesla
Rajiv Ramasawmy*1,2, Thomas Roberts*1,3,
Bernard Siow1, Sean Peter Johnson1,2,
Jack Anthony Wells1, Alan Bainbridge4,
Rosamund Barbara Pedley2, Mark Francis
Lythgoe†1, and Simon Walker-Samuel†1
1Centre for Advanced Biomedical Imaging,
University College London, London, Greater London,
United Kingdom, 2Cancer
Institute, University College London, London, Greater
London, United Kingdom, 3Centre
for Mathematics and Physics in the Life Sciences and
Experimental Biology, University College London, London,
Greater London, United Kingdom, 4Department
of Medical Physics, University College London, London,
Greater London, United Kingdom
Low-field pre-clinical MRI scanners offer economical
imaging of small animal models of cancer, although
whether they provide sufficient signal-to-noise for the
detection of tumours within reasonable imaging times is
currently unknown. In this study, tumour and liver
volumes were measured in a mouse model of liver
metastasis using a 1T bench-top MRI system and a 9.4T
scanner. Volumetric comparison was performed, alongside
signal-to-noise characterisation and contrast assessment
between tumour and liver. T1 and T2 mapping is also
reported. Volumetric analysis of livers and tumours
showed good correspondence, suggesting that bench-top
MRI scanners potentially offer a cost-effective platform
for accurately monitoring deep-seated tumour models and
liver diseases.
|
1154. |
In-Vitro Detection
of Apoptosis Using Oscillating and Pulsed Gradient Diffusion
Magnetic Resonance Imaging
Sharon Portnoy1, Nicole D. Fichtner2,
Claudia Dziegielewski1, Martin P. Stanisz1,
and Greg J. Stanisz1,2
1Sunnybrook Research Institute, Toronto,
Ontario, Canada, 2Department
of Medical Biophysics, University of Toronto, Ontario,
Canada
A wide range of diffusion experiments and a simple model
of diffusion in tissues were used to probe the
microstructural effects of apoptosis. Experiments were
conducted on acute myeloid leukemia (AML) cell pellets,
where apoptosis was induced by treatment with the
chemotherapeutic agent, cisplatin. Seventy-two hours
following treatment pulsed (PGSE) and oscillating (OGSE)
gradient diffusion measurements were performed to assess
effects across a broad range of structural scales. The
presence of apoptosis,which was confirmed by histology,
significantly altered diffusion properties.
|
1155. |
A feasibility study of
diffusion MRI for early detection of xenograft models in
mice.
Paola Porcari1,2, Monika E Hegi3,
Hongxia Lei1, Marie-France Hamou3,
Irene Vassallo3, Silvia Capuani4,5,
Rolf Gruetter1,6, and Vladimir Mlynarik1,7
1Center for Biomedical Imaging, Ecole
Polytechnique Fédérale de Lausanne, Lausanne,
Switzerland, 2Newcastle
Magnetic Resonance Centre, Newcastle University,
Newcastle upon Tyne, United Kingdom, 3Clinical
Neurosciences, Laboratory of Brain Tumor Biology and
Genetics, Lausanne University Hospital and University of
Lausanne, Lausanne, Switzerland, 4CNR-IPCF
UOS Roma Sapienza, Physics Department, Sapienza
University of Rome, Rome, Italy, 5Center
for Life Nanoscience@Sapienza, Istituto Italiano di
Tecnologia, Rome, Italy, 6Departments
of Radiology, Universities of Lausanne and Geneva,
Switzerland, 7High
Field MR Center, Medical University of Vienna, Vienna,
Austria
In this study, high sensitivity and specificity of
diffusion MRI methods for early detection of slow
growing and highly infiltrative tumours, otherwise not
visible in conventional T2-weighted images, haves been
demonstrated. In contrast to conventional MRI, tumours
grown as human glioma sphere xenografts in mice were
identified and investigated in the early stages, and
confirmed by proton MR spectroscopy and
immunohistochemistry. Differences in diffusion
properties of each xenograft highlighted diverse tumour
microstructures which were notably reflected by
histology.
|
1156. |
Identification of Early
Stage Glioblastoma Multiform in Rats by Multi-parametric MR
Imaging Techniques: Preliminary Results
Xu Han1,2, Hua Guo2, Le He2,
Xiaodong Ma2, Tingting Ha3, Kai
Wang4, Yanfeng Xu5, Jianming Cai1,
and Xihai Zhao2
1Department of Radiology, Chinese PLA general
hospital, Beijing, China, 2Center
for Biomedical Imaging Research & Department of
Biomedical Engineering, Tsinghua University, Beijing,
China, 3Department
of Radiology, Tiantan hospital, Capital Medical
University, Beijing, China, 4Imaging
Center of Neuroscience, Tiantan Hospital, Capital
Medical University, Beijing, China, 5Institute
of Laboratory Animal Sciences, Chinese Academy of
Medical Sciences, Beijing, China
In this study, the preliminary results indicate that the
multi-parametric MR imaging technique is feasible to
identify the GBM in rats at early stage. Compared to the
traditional imaging sequences, each sequence of our
multi-parametric imaging protocol, such as spiral DWI,
VDS-DWI, DCE-MRI and CE-T1W, enables discrimination of
the early stage GBM from post-injury brain edema. For
VDS-DWI, the increase of SNR and removal of distortion
can be also obtained in GBM animal model in our study.
The multi-parametric imaging techniques might be an
alternative imaging approach to detect lesions no matter
in brain or other organs at clinically.
|
1157. |
Longitudinal Generalized
Q-Sampling MRI Evaluation in Rabbit Brain after Cerebral
Hemisphere Radiation Exposure
Chao-Yu Shen1,2, Fang-Yu Nien1,
Zhen-Hui Li1, Yeu-Sheng Tyan1,2,
and Jun-Cheng Weng1,2
1School of Medical Imaging and Radiological
Sciences, Chung Shan Medical University, Taichung,
Taiwan, 2Department
of Medical Imaging, Chung Shan Medical University
Hospital, Taichung, Taiwan
Radiation therapy is widely used for the treatment of
both primary and metastatic brain tumors and can lead to
cellular, vascular and axonal injury and further
behavioral deficits. Imaging assessment of the brain
damage caused by radiation therapy is very important for
determining patient prognoses. Previously we used
diffusion tensor imaging (DTI) and T2-weighted imaging
(T2WI) to evaluate post-irradiation brain injury. To
improve evaluation of the neuro-toxic adverse effects of
irradiation treatment in both gray and white matter
structures, in this study we longitudinally evaluated
the changes in various brain compartments on a clinical
MR scanner by using generalized q-sampling imaging (GQI)
indices mappings, generalized fractional anisotropy (GFA),
quantitative anisotropy (QA) and isotropic value (ISO)
of the orientation distribution function (ODF), for
single sub-lethal high dose (30 Gy) cerebral hemisphere
exposure radiation-induced brain injury on adult rabbit
model.
|
1158. |
Exploring the Biomechanical
Properties of Brain Malignancies and their Pathological
Determinants with Magnetic Resonance Elastography
Jin Li1, Yann Jamin1, Jessica K.R.
Boult1, Philippe Garteiser2, Jose
L. Ulloa3, Sergey Popov4,5, Craig
Cummings1, Gary Box5, Suzanne A.
Eccles5, Chris Jones4,5, John C.
Waterton3, Jeffrey C. Bamber1,
Ralph Sinkus2,6, and Simon P. Robinson1
1Division of Radiotherapy & Imaging, The
Institute of Cancer Research, Sutton, Surrey, United
Kingdom, 2INSERM
U773, CRB3, Centre de Recherches Biomédicales
Bichat-Beaujon, France, 3Personalised
Healthcare and Biomarkers, AstraZeneca, Macclesfield,
Cheshire, United Kingdom, 4Division
of Molecular Pathology, The Institute of Cancer
Research, Sutton, Surrey, United Kingdom, 5Division
of Cancer Therapeutics, The Institute of Cancer
Research, Sutton, Surrey, United Kingdom, 6BHF
Centre of Excellence, Division of Imaging Sciences and
Biomedical Engineering, King's College London, King's
Health Partners, St Thomas' Hospital, London, United
Kingdom
Recently MRE revealed that tumours derived from human
breast adenocarcinoma MDA-MB-231, rat Glioma RG2 or
human gioblastoma U87-MG cells were softer than healthy
brain tissue, with MDA-MB-231 significantly softer and
less viscous than the other two models. We investigated
the cellular density, microvessel density, myelin
content and collagen content in these models, and showed
that between the tumours, in MDA-MB-231 tumours, cell
density and microvessel density were significantly lower
than the other two models, positive correlated with
MRE-derived elasticity and viscosity. Meanwhile, the
lack of anisotropic structure of intracranial tumours
may underpin their relative softness.
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1159. |
Is the reaction-diffusion
equation an accurate model of C6 glioma growth?
David A. Hormuth, II1,2, Jared A. Weis2,
and Thomas E. Yankeelov2
1Biomedical Engineering, Vanderbilt
University, Nashville, TN, United States, 2Institute
of Imaging Science, Vanderbilt University, Nashville,
TN, United States
The reaction-diffusion equation is a common model used
to describe tumor growth. Quantitative imaging
measurements may be used to drive this model. Using
simulated tumor growths and experimentally measured
tumor growths, we determined the acquisition strategies
necessary to allow for accurate estimate of model
parameters. Additionally, the accuracy of this model in
predicting in vivo tumor growth is tested. The accuracy
of predicted and observed growths are compared between
the simulated and experimental datasets.
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1160. |
Multiparametric
characterization of the sex differences in a high-grade
glioma rat model by in vivo magnetic resonance and
post-mortem analysis.
Rocio Perez-Carro1, Omar Cauli2,
and Pilar Lopez-Larrubia1
1Department of Experimental models of human
diseases, Instituto de Investigaciones Biomédicas,
CSIC-UAM, Madrid, Spain, 2Department
of Nursing, University of Valencia, Valencia, Spain
Despite there is a clear predominance in cerebral tumors
in male, gender differences are not usually considered
either in the behavioural characterization or new
therapies development in brain oncology. In the present
work we used an animal model of high-grade glioma to
assess in vivo and ex vivo the gender dependence of MR
and biological parameters. Glioma bearing female rats
showed more extended necrosis in tumors than males,
while the latters present higher disruption of the blood
brain barrier. We indicate the ability of using MR
surrogate markers to signal and track the gender
dependence in brain tumorigenesis.
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1161.
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Tracking tissue oxygenation
status and response using Diffusion-Weighted functional MRI
Zhongwei Zhang1, Rami R Hallac1,
Qing Yuan1, Peter Peschke2, and
Ralph P Mason1
1Department of Radiology, The University of
Texas Southwestern Medical Center, Dallas, TX, United
States, 2Clinical
Cooperation Unit Radiation Oncology, German Cancer
Research Center, Heidelberg, Germany
The diffusion-sensitized fMRI (DfMRI) has the potential
to provide noninvasive measurements of tissue
oxygenation using oxygen as an endogenous paramagnetic
contrast agent, in this study, we compared DfMRI
response with BOLD, TOLD responses to gas breathing
challenge under different baseline pO2 level. The
feasibility of DfMRI for tracking tissue oxygenation
status was evaluated. Our study showed that DfMRI is a
powerful tool to tracking tissue oxygenation status and
it can also provide the extent of response when
combining baseline pO2 measurement.
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1162. |
On conductivity,
permittivity, apparent diffusion coefficients and their use
as cancer markers at MRI frequencies
Ileana Hancu1, Jeanette Roberts1,
Seung-Kyun Lee1, Robert Lenkinski2,
and Selaka Bulumulla1
1GE Global Research Center, Niskayuna, NY,
United States, 2UT
Southwestern Medical Center, TX, United States
Experiments using an impedance analyzer/dielectric probe
were performed in two rat cancer models to validate the
frequency dependant differences in tissue electrical
properties (TEP's) between cancer and normal tissues.
Correlations between conductivity and apparent diffusion
coefficient (ADC) were also investigated. While it was
found that limited differences (5-30%) exist between the
TEP's of cancer and normal tissue, permittivity added
significant discriminant power compared to ADC alone,
particularly at 1.5T and 3T. If MRI based TEP
measurements could be brought to ~5%
accuracy/repeatability, it is suggested that 3T exams
involving ADC and permittivity mapping could better
discern cancer from normal tissue.
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1163. |
PEG-masked ferritin-based
multifunctional nanoparticles in melanoma murine model
Giulia Carpinelli1, Rossella Canese1,
Elisabetta Falvo2, Cristina Maria Failla3,
Miriam Carbo2, Manuela Fornara4,
Serena Cecchetti1, Lenka Rajsiglova5,
Dmitry Stakheev5, Jiri Krizan5,
Alberto Boffi2,4, Veronica Morea2,
Luca Vannucci5, and Pierpaolo Ceci2
1Cell Biology and Neurosciences Dept,
Istituto Superiore di Sanità, Rome, Italy, 2Institute
of Molecular Biology and Pathology, CNR – National
Research Council of Italy, Rome, Italy, 3Molecular
and Cell Biology Laboratory, IDI-IRCCS, Rome, Italy, 4Department
of Biochemical Sciences “A. Rossi Fanelli”, University
of Rome “Sapienza”, Rome, Italy, 5Institute
of Microbiology, Academy of Sciences of the Czech
Republic (ASCR), Prague, Czech Republic
Nanoparticles (NPs) are promising agents for enhancing
cancer diagnosis and treatment. Once functionalized for
selective targeting of tumor expressed molecules, they
can specifically deliver drugs and diagnostic molecules
inside tumor cells. We evaluated the in vivo
melanoma-targeting ability of a nanovector (HFt-MSH-PEG)
based on human protein ferritin (HFt), functionalized
with both melanoma-targeting melanoma stimulating
hormone (α-MSH) and stabilizing poly(ethylene glycol)
molecules, with magnetite-maghemite encapsulation. NPs
showed by MRI an accumulation in primary melanoma, with
high selectivity with respect to other organs, thereby
proving to be suitable vectors for selective delivery of
diagnostic or therapeutic agents for cutaneous melanoma.
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1164. |
A Novel Gd-Sucrose Scaffold
for Oral Administration in MR-colonography at 7 T
Parastou Foroutan1, Gary V Martinez1,
Valerie E Moberg1, Suryakiran Navath2,
Robert J Gillies1, Eugene A Mash2,
and David L Morse1
1Cancer Imaging & Metabolism, H. Lee Moffitt
Cancer Center & Research Institute, Tampa, FL, United
States, 2Department
of Chemistry and Biochemistry, University of Arizona,
Tucson, Arizona, United States
Colorectal cancer (CRC) is the second leading cause of
death in the United States and although CRC prognosis
relies on early-stage-disease detection, the standard
screening method, colonoscopy, suffers from patient
non-compliance. Magnetic resonance colonography (MR-C)
is a non-invasive approach that provides excellent soft
tissue contrast and 3D datasets without radiation
exposure. Herein, we present the development of targeted
contrast agents for pre-screening of CRC by 7 T MRI.
Specifically, a non-toxic Gd-DOTA sucrose based scaffold
for oral administration that can be conjugated to
targeting moieties specific for CRC was developed and
evaluated in phantoms as well as in vivo in xenografts.
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1165. |
Assessment of the tumoral
microenvironment in the development of a glioblastoma rat
model by in vivo MRI and ex vivo HRMAS
Ana Amor-López1, Rocío Pérez-Carro1,
and Pilar López-Larrubia1
1Instituto de Investigaciones Biomédicas
"Alberto Sols", CSIC-UAM, Madrid, Madrid, Spain
Current techniques for evaluating microvasculature and
inflammatory processes linked to cancer development, do
not achieve an enough spatial and functional resolution,
bordering the applications both for diagnosis and
therapy validation. Magnetic resonance imaging and
spectroscopy approaches offer a great potential to
solving these limitations. In fact, MR approaches allow
determining important characteristics of tumor
microenvironment as microvascular abnormalities, tumor
metabolism, oxygenation level and extracellular-pH
between others. This research was focussed on the
identification of MR parameters that may act as in vivo
surrogate markers of biological characteristic -like
inflammation, edema and BBB integrity- of a glioblastoma
in a rat model.
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