基于离体100μm各向同性扩散MRI的亨廷顿舞蹈症终末期R6/2小鼠模型连接变化的束描记术。

Neuroprotection Pub Date : 2023-09-01 Epub Date: 2022-12-20 DOI:10.1002/nep3.14
Ashwinee Manivannan, Lesley M Foley, T Kevin Hitchens, Ivan Rattray, Gillian P Bates, Michel Modo
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摘要

背景:亨廷顿舞蹈症是一种进行性神经退行性疾病。体积磁共振成像(MRI)测量的脑萎缩是神经退行性变的下游后果,但脑组织内的微观结构变化预计会先于这种体积下降。组织微观结构可以使用扩散MRI进行非侵入性分析,这也允许对大脑连接进行牵引图分析。方法:我们使用离体扩散MRI(11.7T)来测量终末期(14周龄)野生型和R6/2小鼠(雄性和雌性)亨廷顿舞蹈症模型不同大脑区域的微观结构变化。为了探测不同大脑区域的微观结构,减少部分体积效应,并测量不同区域之间的连通性,获得了100μm的各向同性体素分辨率。结果:尽管部分各向异性在野生型对照和R6/2小鼠之间没有显示出任何差异,但雌性R6/2小鼠的平均、轴向和径向扩散率增加,而雄性R6/2小鼠则降低。全脑流线仅在雄性R6/2小鼠中减少,但流线密度增加。区域间束描记术显示皮层、海马体和丘脑与纹状体之间以及基底神经节(纹状体苍白球-丘脑底核-黑质-丘脑)内的连通性降低。结论:生物性别和左/右半球影响束描记结果,可能反映疾病进展的不同阶段。这项原理验证研究表明,扩散MRI和束描记术可能提供新的生物标志物,将不同大脑区域的体积变化联系起来。在翻译环境中,这些测量构成了一种新的工具,可以评估转基因模型中的神经保护剂等干预措施以及亨廷顿舞蹈症患者的治疗效果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Ex vivo 100 μm isotropic diffusion MRI-based tractography of connectivity changes in the end-stage R6/2 mouse model of Huntington's disease.

Background: Huntington's disease is a progressive neurodegenerative disorder. Brain atrophy, as measured by volumetric magnetic resonance imaging (MRI), is a downstream consequence of neurodegeneration, but microstructural changes within brain tissue are expected to precede this volumetric decline. The tissue microstructure can be assayed non-invasively using diffusion MRI, which also allows a tractographic analysis of brain connectivity.

Methods: We here used ex vivo diffusion MRI (11.7 T) to measure microstructural changes in different brain regions of end-stage (14 weeks of age) wild type and R6/2 mice (male and female) modeling Huntington's disease. To probe the microstructure of different brain regions, reduce partial volume effects and measure connectivity between different regions, a 100 μm isotropic voxel resolution was acquired.

Results: Although fractional anisotropy did not reveal any difference between wild-type controls and R6/2 mice, mean, axial, and radial diffusivity were increased in female R6/2 mice and decreased in male R6/2 mice. Whole brain streamlines were only reduced in male R6/2 mice, but streamline density was increased. Region-to-region tractography indicated reductions in connectivity between the cortex, hippocampus, and thalamus with the striatum, as well as within the basal ganglia (striatum-globus pallidus-subthalamic nucleus-substantia nigra-thalamus).

Conclusions: Biological sex and left/right hemisphere affected tractographic results, potentially reflecting different stages of disease progression. This proof-of-principle study indicates that diffusion MRI and tractography potentially provide novel biomarkers that connect volumetric changes across different brain regions. In a translation setting, these measurements constitute a novel tool to assess the therapeutic impact of interventions such as neuroprotective agents in transgenic models, as well as patients with Huntington's disease.

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