Huang Susie Y, Nummenmaa Aapo, Witzel Thomas, Duval Tanguy, Cohen-Adad Julien, Wald Lawrence L, McNab Jennifer A
Athinoula A. Martinos Center for Biomedical Imaging, Department of Radiology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, United States.
Athinoula A. Martinos Center for Biomedical Imaging, Department of Radiology, Massachusetts General Hospital, Harvard Medical School, Boston, MA, United States.
Neuroimage. 2015 Feb 1;106:464-72. doi: 10.1016/j.neuroimage.2014.12.008. Epub 2014 Dec 9.
Diffusion magnetic resonance imaging (MRI) methods for axon diameter mapping benefit from higher maximum gradient strengths than are currently available on commercial human scanners. Using a dedicated high-gradient 3T human MRI scanner with a maximum gradient strength of 300 mT/m, we systematically studied the effect of gradient strength on in vivo axon diameter and density estimates in the human corpus callosum. Pulsed gradient spin echo experiments were performed in a single scan session lasting approximately 2h on each of three human subjects. The data were then divided into subsets with maximum gradient strengths of 77, 145, 212, and 293 mT/m and diffusion times encompassing short (16 and 25 ms) and long (60 and 94 ms) diffusion time regimes. A three-compartment model of intra-axonal diffusion, extra-axonal diffusion, and free diffusion in cerebrospinal fluid was fitted to the data using a Markov chain Monte Carlo approach. For the acquisition parameters, model, and fitting routine used in our study, it was found that higher maximum gradient strengths decreased the mean axon diameter estimates by two to three fold and decreased the uncertainty in axon diameter estimates by more than half across the corpus callosum. The exclusive use of longer diffusion times resulted in axon diameter estimates that were up to two times larger than those obtained with shorter diffusion times. Axon diameter and density maps appeared less noisy and showed improved contrast between different regions of the corpus callosum with higher maximum gradient strength. Known differences in axon diameter and density between the genu, body, and splenium of the corpus callosum were preserved and became more reproducible at higher maximum gradient strengths. Our results suggest that an optimal q-space sampling scheme for estimating in vivo axon diameters should incorporate the highest possible gradient strength. The improvement in axon diameter and density estimates that we demonstrate from increasing maximum gradient strength will inform protocol development and encourage the adoption of higher maximum gradient strengths for use in commercial human scanners.
用于轴突直径测绘的扩散磁共振成像(MRI)方法受益于比目前商用人体扫描仪更高的最大梯度强度。我们使用一台最大梯度强度为300 mT/m的专用高梯度3T人体MRI扫描仪,系统地研究了梯度强度对人体胼胝体体内轴突直径和密度估计的影响。在三个受试者中的每一个身上,在一次持续约2小时的单次扫描中进行了脉冲梯度自旋回波实验。然后将数据分为最大梯度强度分别为77、145、212和293 mT/m的子集,扩散时间涵盖短(16和25毫秒)和长(60和94毫秒)扩散时间范围。使用马尔可夫链蒙特卡罗方法将轴突内扩散、轴突外扩散和脑脊液中自由扩散的三室模型拟合到数据中。对于我们研究中使用的采集参数、模型和拟合程序,发现更高的最大梯度强度使整个胼胝体的平均轴突直径估计值降低了两到三倍,并将轴突直径估计值的不确定性降低了一半以上。仅使用较长的扩散时间导致轴突直径估计值比使用较短扩散时间时大两倍。轴突直径和密度图的噪声似乎更小,并且在更高的最大梯度强度下,胼胝体不同区域之间的对比度得到改善。胼胝体膝部、体部和压部之间已知的轴突直径和密度差异得以保留,并且在更高的最大梯度强度下变得更具可重复性。我们的结果表明,用于估计体内轴突直径的最佳q空间采样方案应包含尽可能高的梯度强度。我们通过提高最大梯度强度所展示的轴突直径和密度估计的改善将为方案制定提供参考,并鼓励在商用人体扫描仪中采用更高的最大梯度强度。
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