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高 b 值弥散张量成像在多发性硬化症小鼠模型中海马亚结构早期改变中的应用。

High B-value diffusion tensor imaging for early detection of hippocampal microstructural alteration in a mouse model of multiple sclerosis.

机构信息

INSERM, U1215, Neurocentre Magendie, 33000, Bordeaux, France.

University of Bordeaux, 33000, Bordeaux, France.

出版信息

Sci Rep. 2022 Jul 14;12(1):12008. doi: 10.1038/s41598-022-15511-0.

Abstract

Several studies have highlighted the value of diffusion tensor imaging (DTI) with strong diffusion weighting to reveal white matter microstructural lesions, but data in gray matter (GM) remains scarce. Herein, the effects of b-values combined with different numbers of diffusion-encoding directions (NDIRs) on DTI metrics to capture the normal hippocampal microstructure and its early alterations were investigated in a mouse model of multiple sclerosis (experimental autoimmune encephalomyelitis [EAE]). Two initial DTI datasets (B2700-43Dir acquired with b = 2700 s.mm and NDIR = 43; B1000-22Dir acquired with b = 1000 s.mm and NDIR = 22) were collected from 18 normal and 18 EAE mice at 4.7 T. Three additional datasets (B2700-22Dir, B2700-12Dir and B1000-12Dir) were extracted from the initial datasets. In healthy mice, we found a significant influence of b-values and NDIR on all DTI metrics. Confronting unsupervised hippocampal layers classification to the true anatomical classification highlighted the remarkable discrimination of the molecular layer with B2700-43Dir compared with the other datasets. Only DTI from the B2700 datasets captured the dendritic loss occurring in the molecular layer of EAE mice. Our findings stress the needs for both high b-values and sufficient NDIR to achieve a GM DTI with more biologically meaningful correlations, though DTI-metrics should be interpreted with caution in these settings.

摘要

几项研究强调了使用强扩散加权的扩散张量成像(DTI)来揭示白质微观结构病变的价值,但灰质(GM)的数据仍然很少。在此,研究了 b 值与不同扩散编码方向数(NDIR)相结合对 DTI 指标的影响,以捕获多发性硬化症(实验性自身免疫性脑脊髓炎[EAE])小鼠模型中的正常海马微观结构及其早期改变。在 4.7 T 下,从 18 只正常和 18 只 EAE 小鼠中收集了两个初始 DTI 数据集(b = 2700 s.mm 和 NDIR = 43 的 B2700-43Dir 采集;b = 1000 s.mm 和 NDIR = 22 的 B1000-22Dir 采集)。从初始数据集提取了另外三个数据集(B2700-22Dir、B2700-12Dir 和 B1000-12Dir)。在健康小鼠中,我们发现 b 值和 NDIR 对所有 DTI 指标都有显著影响。将无监督的海马层分类与真实解剖分类进行比较,突出了 B2700-43Dir 与其他数据集相比对分子层的显著区分。只有 B2700 数据集的 DTI 才能捕捉到 EAE 小鼠分子层中发生的树突丢失。我们的研究结果强调了需要高 b 值和足够的 NDIR 来实现具有更有生物学意义相关性的 GM DTI,但在这些情况下应谨慎解释 DTI 指标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b707/9283448/88e856f229b0/41598_2022_15511_Fig1_HTML.jpg

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