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  4. Diffusion-Weighted Spectroscopy: A Novel Approach to Determine Macromolecule Resonances in Short-Echo Time H-1-MRS
 
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research article

Diffusion-Weighted Spectroscopy: A Novel Approach to Determine Macromolecule Resonances in Short-Echo Time H-1-MRS

Kunz, N.  
•
Cudalbu, Cristina Ramona  
•
Mlynarik, V.  
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2010
Magnetic Resonance In Medicine

Quantification of short-echo time proton magnetic resonance spectroscopy results in >18 metabolite concentrations (neurochemical profile). Their quantification accuracy depends on the assessment of the contribution of macromolecule (MM) resonances, previously experimentally achieved by exploiting the several fold difference in T-1. To minimize effects of hetero-geneities in metabolites T-1, the aim of the study was to assess MM signal contributions by combining inversion recovery (IR) and diffusion-weighted proton spectroscopy at high-magnetic field (14.1 T) and short echo time (=8 msec) in the rat brain. IR combined with diffusion weighting experiments (with delta/Delta = 1.5/200 msec and b-value = 11.8 msec/mu m(2)) showed that the metabolite nulled spectrum (inversion time = 740 msec) was affected by residuals attributed to creatine, inositol, taurine, choline, N-acetylaspartate as well as glutamine and glutamate. While the metabolite residuals were significantly attenuated by 50%, the MM signals were almost not affected (<8%). The combination of metabolite-nulled IR spectra with diffusion weighting allows a specific characterization of MM resonances with minimal metabolite signal contributions and is expected to lead to a quantification of the neurochemical profile. Med 64:939-946, 2010. (C) 2010 Wiley-Liss, Inc.

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Type
research article
DOI
10.1002/mrm.22490
Web of Science ID

WOS:000282477100002

Author(s)
Kunz, N.  
•
Cudalbu, Cristina Ramona  
•
Mlynarik, V.  
•
Hueppi, P. S.
•
Sizonenko, S. V.
•
Gruetter, R.  
Date Issued

2010

Publisher

Wiley-Blackwell

Published in
Magnetic Resonance In Medicine
Volume

64

Start page

939

End page

946

Subjects

proton magnetic resonance spectroscopy

•

macromolecules

•

ultra-high field of 14.1 T

•

LCModel

•

quantification accuracy

•

Brain In-Vivo

•

Rat-Brain

•

Neurochemical Profile

•

T-2 Relaxation

•

Metabolite Concentrations

•

H-1-Nmr Spectra

•

14.1 Tesla

•

Base-Line

•

Quantification

•

Signals

•

CIBM-AIT

Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
CIBM  
LIFMET  
Available on Infoscience
December 16, 2011
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/75115
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