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Post-mortem inference of the human hippocampal connectivity and microstructure using ultra-high field diffusion MRI at 11.7 T

机译:使用11.7 T的超高场扩散MRI进行人体海马连通性和微观结构的事后推断

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摘要

The human hippocampus plays a key role in memory management and is one of the first structures affected by Alzheimer’s disease. Ultra-high magnetic resonance imaging provides access to its inner structure in vivo. However, gradient limitations on clinical systems hinder access to its inner connectivity and microstructure. A major target of this paper is the demonstration of diffusion MRI potential, using ultra-high field (11.7 T) and strong gradients (750 mT/m), to reveal the extra- and intra-hippocampal connectivity in addition to its microstructure. To this purpose, a multiple-shell diffusion-weighted acquisition protocol was developed to reach an ultra-high spatio-angular resolution with a good signal-to-noise ratio. The MRI data set was analyzed using analytical Q-Ball Imaging, Diffusion Tensor Imaging (DTI), and Neurite Orientation Dispersion and Density Imaging models. High Angular Resolution Diffusion Imaging estimates allowed us to obtain an accurate tractography resolving more complex fiber architecture than DTI models, and subsequently provided a map of the cross-regional connectivity. The neurite density was akin to that found in the histological literature, revealing the three hippocampal layers. Moreover, a gradient of connectivity and neurite density was observed between the anterior and the posterior part of the hippocampus. These results demonstrate that ex vivo ultra-high field/ultra-high gradients diffusion-weighted MRI allows the mapping of the inner connectivity of the human hippocampus, its microstructure, and to accurately reconstruct elements of the polysynaptic intra-hippocampal pathway using fiber tractography techniques at very high spatial/angular resolutions.Electronic supplementary materialThe online version of this article (10.1007/s00429-018-1617-1) contains supplementary material, which is available to authorized users.
机译:人海马在记忆管理中起着关键作用,是受阿尔茨海默氏病影响的首批结构之一。超高磁共振成像可在体内访问其内部结构。但是,临床系统的梯度限制阻碍了其内部连通性和微观结构的获取。本文的主要目标是利用超高场(11.7 T)和强梯度(750 mT / m)来演示弥散MRI的潜力,以揭示其微结构之外的海马外和海马内部连通性。为此,开发了一种多壳扩散加权采集协议,以达到具有极佳信噪比的超高空间角度分辨率。 MRI数据集使用分析Q球成像,扩散张量成像(DTI)和神经突取向分散和密度成像模型进行了分析。高角分辨率扩散成像估计值使我们能够获得比DTI模型更复杂的光纤架构的精确束线照相术,并随后提供了跨区域连接的地图。神经突密度类似于组织学文献中发现的神经突密度,揭示了三个海马层。此外,在海马的前部和后部之间观察到连通性和神经突密度的梯度。这些结果表明,离体超高场/超高梯度扩散加权MRI可以绘制人海马的内部连通性,其微结构,并使用纤维束摄影技术准确地重建多突触海马通路的元素电子补充材料本文的在线版本(10.1007 / s00429-018-1617-1)包含补充材料,授权用户可以使用。

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