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体内前列腺 ¹H-MRSI 的短回波时间。

Short echo time in vivo prostate ¹H-MRSI.

机构信息

Department of Physics and Astronomy, University of Manitoba, Winnipeg, Manitoba, Canada.

出版信息

Magn Reson Imaging. 2012 Feb;30(2):195-204. doi: 10.1016/j.mri.2011.09.020. Epub 2011 Dec 9.

DOI:10.1016/j.mri.2011.09.020
PMID:22154684
Abstract

Visualization of short echo time (TE) metabolites in prostate magnetic resonance spectroscopic imaging is difficult due to lipid contamination and pulse timing constraints. In this work, we present a modified pulse sequence to permit short echo time (TE=40ms) acquisitions with reduced lipid contamination for the detection of short TE metabolites. The modified pulse sequence employs the conformal voxel MRS (CV-MRS) technique, which automatically optimizes the placement of spatial saturation planes to adapt the excitation volume to the shape of the prostate, thus reducing lipid contamination in prostate magnetic resonance spectroscopic imaging (MRSI). Metabolites were measured and assessed using a modified version of LCModel for analysis of in vivo prostate spectra. We demonstrate the feasibility of acquiring high quality spectra at short TEs, and show the measurement of short TE metabolites, myo-inositol, scyllo-inositol, taurine and glutamine/glutamate for both single and multi-voxel acquisitions. In single voxels experiments, the reduction in TE resulted in 57% improvement in the signal-to-noise ratio (SNR). Additional 3D MRSI experiments comparing short (TE=40 ms), and long (TE=130 ms) TE acquisitions revealed a 35% improvement in the number of adequately fitted metabolite peaks (775 voxels over all subjects). This resulted in a 42 ± 24% relative improvement in the number of voxels with detectable citrate that were well-fitted using LCmodel. In this study, we demonstrate that high quality prostate spectra can be obtained by reducing the TE to 40 ms to detect short T2 metabolites, while maintaining positive signal intensity of the spin-coupled citrate multiplet and managing lipid suppression.

摘要

由于脂质污染和脉冲定时限制,前列腺磁共振波谱成像中短回波时间 (TE) 代谢物的可视化较为困难。在这项工作中,我们提出了一种改进的脉冲序列,可在减少脂质污染的情况下实现短回波时间 (TE=40ms) 采集,以检测短 TE 代谢物。改进的脉冲序列采用共形体素 MRS(CV-MRS)技术,该技术自动优化空间饱和平面的放置位置,以适应前列腺的形状,从而减少前列腺磁共振波谱成像 (MRSI) 中的脂质污染。代谢物的测量和评估使用 LCModel 的修改版本进行,用于分析体内前列腺谱。我们证明了在短 TE 下获取高质量谱的可行性,并展示了单和多体素采集时短 TE 代谢物肌醇、船形肌醇、牛磺酸和谷氨酰胺/谷氨酸的测量结果。在单体素实验中,TE 的减少使信噪比 (SNR) 提高了 57%。比较短(TE=40ms)和长(TE=130ms)TE 采集的附加 3D MRSI 实验表明,代谢物峰拟合良好的数量增加了 35%(所有受试者共有 775 个体素)。这使得使用 LCmodel 可检测到柠檬酸的拟合良好的体素数量相对增加了 42±24%。在这项研究中,我们证明通过将 TE 降低到 40ms 可以获得高质量的前列腺谱,以检测短 T2 代谢物,同时保持自旋偶合柠檬酸多重峰的正信号强度并管理脂质抑制。

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