10:30 |
0736. |
Introduction
Elena Vinogradov
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10:42 |
0737.
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Imaging of Glutamate in
the Spinal Cord using Chemical Exchange Saturation Transfer
(CEST) at 7T
Feliks Kogan1,2, Anup Singh1,
Mohammad Haris1, Kejia Cai1, Hari
Hariharan1, and Ravinder Reddy1
1Center for Magnetic Resonance and Optical
Imaging, University of Pennsylvania, Philadelphia, PA,
United States, 2Bioengineering
Graduate Group, University of Pennsylvania,
Philadelphia, PA, United States
Glutamate (Glu) is the primary neurotransmitter that is
responsible for excitatory synaptic transmission in the
brain stem and spinal cord and plays a wide role in
neuropathology. Glu exhibits a CEST effect which is
linearly proportional to the Glu concentration. In this
work, we demonstrated that it is feasible to detect the
CEST effect from glutamate in the cervical spinal cord
at 7T with high spatial resolution. We showed that the
spinal cord Glu CEST map demonstrates a distinct gray
and white matter distribution pattern. Finally, we
demonstrated from phantom data that the majority of the
CEST contrast in the spinal cord is due to glutamate.
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10:54 |
0738. |
Imaging acute ischemic
tissue acidosis with quantitative in vivo amide proton
transfer (APT) MRI
Phillip Zhe Sun1, Enfeng Wang1,
and Jerry S Cheung1
1Department of Radiology, Athinoula A.
Martinos Center for Biomedical Imaging, Charlestown, MA,
United States
Amide proton transfer (APT) MRI is capable of imaging
tissue acidosis during acute stroke. However,
magnetization transfer asymmetry (MTRasym) is often
calculated for pH-weighted APT contrast, which is
subject to a baseline shift (ÄMTR’asym) attributable to
the slightly asymmetric magnetization transfer (MT)
effect. In this study, we modeled MTRasym as a
superposition of pH-dependent APT contrast and a
baseline shift ÄMTR’asym (i.e., MTRasym=APTR(pH) +
ÄMTR’asym). We found schemic lesion pH was 6.44 ± 0.24,
significantly reduced from that of the normal tissue
(7.03 ± 0.05), which correlated with tissue perfusion
and diffusion rates.
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11:06 |
0739. |
Quantitative MR imaging of
the Amide-proton transfer, the Nuclear Overhauser effect,
and MT asymmetry: a 9.4 T study
Tao Jin1, Xiaopeng Zong1, Ping
Wang1, and Seong-Gi Kim1
1Department of Radiology, University of
Pittsburgh, Pittsburgh, Pennsylvania, United States
The amide proton transfer (APT) effect has shown great
potential in stroke and cancer studies. However,
quantitative imaging of the APT effect is still
challenging. The magnitude of APT is typically assessed
from an MTR asymmetry image, which may have
contamination from the conventional MT asymmetry and the
Nuclear Overhauser effect (NOE). In this report, the
wide spectral separation from the high field of 9.4 T is
utilized to obtain quantitative APT and NOE images
without using the asymmetry analysis. We found that pure
APT contrast is highly sensitive to pH, while the NOE
map has little tissue and pH contrast.
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11:18 |
0740.
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Separating CEST from MT
asymmetry by simultaneous two-frequency irradiation
Jae-Seung Lee1,2, Ravinder R Regatte1,
and Alexej Jerschow2
1Department of Radiology, NYU Langone Medical
Center, New York, NY, United States, 2Department
of Chemistry, New York University, New York, NY, United
States
CEST and MT contrast have enjoyed wide popularity
recently in MRI applications. It is often difficult to
separate genuine CEST signatures from MT effects, which
are asymmetric with respect to the water resonance. We
recently developed a method that utilizes simultaneous
two-frequency rf irradiation, which can make MT effects
independent of irradiation frequencies over a wide
range, and thus can suppress MT asymmetry. Based on the
results from the simulations as well as experiments, we
propose a new strategy to isolate CEST contrast from MT
asymmetry contrast by using the two-frequency rf
irradiation technique.
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11:30 |
0741.
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Improved Accuracy of
Cross-Relaxation Imaging Using On-Resonance MT Effect
Correction
Pouria Mossahebi1, Vasily L. Yarnykh2,
and Alexey A. Samsonov3
1Biomedical Engineering, University of
Wisconsin, Madison, WI, United States, 2Radiology,
University of Washington, Seattle, WA, United States, 3Radiology,
University of Wisconsin, Madison, WI, United States
This study demonstrates that separate treatment of VFA
and MT data in the CRI method causes non-negligible
systematic errors in both R1 and cross-relaxation
parameters. Our modified CRI data processing approach
effectively corrects these errors and does not require
any additional measurements, thus maintaining
time-efficiency of the original CRI technique.
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11:42 |
0742. |
In vivo human
kidney pH mapping at 3T using time-interleaved parallel RF
transmission CEST
Ivan E Dimitrov1,2, Masaya Takahashi2,
Koji Sagiyama2, A. Dean Sherry2,3,
and Jochen Keupp4
1Philips Medical Systems, Cleveland, OH,
United States, 2Advanced
Imaging Research Center, University of Texas
Southwestern Medical Center, Dallas, TX, United States, 3Chemistry,
University of Texas Dallas, Richardson, TX, United
States, 4Philips
Research Europe, Hamburg, Germany
A parallel transmission CEST method is presented for
ratiometric, concentration-independent pH mapping of
human kidneys at 3T using clinically approved contrast
agent, Iopamidol. The method combines respiratory
triggered single-shot turbo-spin echo that runs in
time-interleaved mode of an MR scanner with parallel RF
transmission system. Triggering was made such that to
lower the acquisition duty cycle and SAR by skipping
pre-defined number of respiratory cycles to enable
longer and more powerful RF saturation. CEST effects of
up to 20% were recorded in the pelvic and medullar
regions of the kidney, allowing for generating
pixel-wise pH maps.
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11:54 |
0743. |
Interleaved Parallel
Transmission Saturation Scheme for 3D Amide Proton Transfer
Imaging of Brain Tumors at 3 Tesla
He Zhu1,2, Jochen Keupp3, Jaishri
Blakeley4, Lindsay Blair4, Michael
Schar1,5, Peter B. Barker1,2,
Peter C.M. van Zijl1,2, and Jinyuan Zhou1,2
1Department of Radiology, Johns Hopkins
University, Baltimore, Maryland, United States, 2F.M.
Kirby Research Center for Functional Brain Imaging,
Kennedy Krieger Institute, Baltimore, Maryland, United
States, 3Philips
Research, Hamburg, Germany, 4Department
of Neurology, Johns Hopkins University, Baltimore,
Maryland, United States, 5Philips
Healthcare, Cleveland, Ohio, United States
Amide proton transfer (APT) image contrast is generated
by selective RF labeling of amide protons of cytosolic
proteins and peptides in tissue, followed by chemical
exchange of this label to water protons. Currently,
clinical APT imaging protocols are typically limited by
scanner hardware constraints, particularly with respect
to the RF amplifier duty cycle. In this study,
time-interleaved parallel RF transmission (pTX) was used
for 3D APT imaging. The preliminary results show that
the use of the pTX-APT approach can maximize APT-MRI
effects on clinical scanners and that high-quality 3D
APT imaging of human brain tumors can be acquired within
a clinically feasible time.
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12:06 |
0744.
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Effect of Saturation Pulse
Length on Parallel Transmission Based Amide Proton Transfer
(APT) Imaging of Different Brain Tumor Types
Osamu Togao1, Takashi Yoshiura1,
Jochen Keupp2, Akio Hiwatashi1,
Koji Yamashita1, Kazufumi Kikuchi1,
Yuriko Suzuki3, Koji Sagiyama4,
Masaya Takahashi4, and Hiroshi Honda1
1Clinical Radiology, Graduate School of
Medical Science, Kyushu University, Fukuoka, Fukuoka,
Japan, 2Philips
Research, Hamburg, Germany, 3Philips
Electronics, Japan,4Advanced Imaging Research
Center, UT Southwestern Medical Center, Dallas, Texas,
United States
Amide proton transfer (APT) imaging employs the exchange
between protons of free tissue water and the amide
groups (-NH) of endogenous mobile proteins and peptides,
imaged by a saturation transfer technique. In this
imaging technique, the length of RF saturation (Tsat) is
an important parameter for sensitivity. A technique
based on parallel RF transmission was demonstrated,
which allows arbitrarily long RF pulses (~5s) via
amplifier alternation in clinical scanners. We evaluated
the Tsat dependence of the APT contrast in human brain
tumors and to demonstrate the efficacy of long Tsat
achieved by the parallel RF transmission based
technique.
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12:18 |
0745.
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RF Power Dependence of
Human Brain CEST, NOE and Metabolite MT Effects at 7T
Dapeng Liu1, Jinyuan Zhou2,3, Rong
Xue1, Zhentao Zuo1, Jing An4,
and Danny JJ Wang5
1State Key Lab. of Brain and Cognitive
Science, Beijing MRI Center for Brain Research,
Institute of Biophysics, Chinese Academy of Sciences,
Beijing, China, 2FM
Kirby Center, Kennedy Krieger Institute, Baltimore, MD,
United States, 3Department
of Radiology and Radiological Sciences, Johns Hopkins
Medical Institutes, Baltimore, MD, United States, 4Siemens
Shenzhen Magnetic Resonance Ltd, Shenzhen, China, 5Neurology,
UCLA, Los Angeles, CA, United States
In this work we investigated the RF power dependence of
the magnetization transfer (MT) asymmetry effects at 7T.
The results suggest that at low B1, the nuclear
Overhauser enhancement (NOE) and metabolite MT effects
are the dominant source of MT asymmetry while at higher
B1, the amide proton transfer (APT) effect becomes
stronger and finally reverses the asymmetry plot. Our
results suggest that MT asymmetry at 7T with low B1 may
provide an approach for in vivo imaging of brain lipid
(e.g., myelin).
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