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Fast volumetric spatial-spectral MR imaging of hyperpolarized C-labeled compounds using multiple echo 3D bSSFP
Authors:William H Perman  Pratip Bhattacharya  Jochen Leupold  Alexander P Lin  Kent C Harris  Valerie A Norton  Jan-Bernd Hövener  Brian D Ross
Institution:1. Department of Radiology, Saint Louis University School of Medicine, PO Box 15250, St. Louis, MO 63110-0250, USA;2. Huntington Medical Research Institutes, Magnetic Resonance Spectroscopy Section, Pasadena, CA 91105, USA;3. Rudi Schulte Research Institute, PO Box 3130, Santa Barbara, CA 93130-3130, USA;4. A.A. Noyes Laboratory of Chemical Physics, California Institute of Technology, Pasadena, CA 91125, USA;5. Department of Diagnostic Radiology, Medical Physics, University Hospital Freiburg, Hugstetter Str. 55, D-79106 Freiburg, Germany
Abstract:

Purpose

The goal of this work was to develop a fast 3D chemical shift imaging technique for the noninvasive measurement of hyperpolarized 13C-labeled substrates and metabolic products at low concentration.

Materials and Methods

Multiple echo 3D balanced steady state magnetic resonance imaging (ME-3DbSSFP) was performed in vitro on a syringe containing hyperpolarized 1,3,3-2H3; 1-13C]2-hydroxyethylpropionate (HEP) adjacent to a 13C-enriched acetate phantom, and in vivo on a rat before and after intravenous injection of hyperpolarized HEP at 1.5 T. Chemical shift images of the hyperpolarized HEP were derived from the multiple echo data by Fourier transformation along the echoes on a voxel by voxel basis for each slice of the 3D data set.

Results

ME-3DbSSFP imaging was able to provide chemical shift images of hyperpolarized HEP in vitro, and in a rat with isotropic 7-mm spatial resolution, 93 Hz spectral resolution and 16-s temporal resolution for a period greater than 45 s.

Conclusion

Multiple echo 3D bSSFP imaging can provide chemical shift images of hyperpolarized 13C-labeled compounds in vivo with relatively high spatial resolution and moderate spectral resolution. The increased signal-to-noise ratio of this 3D technique will enable the detection of hyperpolarized 13C-labeled metabolites at lower concentrations as compared to a 2D technique.
Keywords:Hyperpolarized 13C  Chemical shift imaging  Balanced steady state free precession imaging  Spectroscopic imaging
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