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p301L tau 诱导的 tau 病小鼠模型的轴突运输障碍及其与弥散张量成像指标的关系。

Axonal Transport Impairment and its Relationship with Diffusion Tensor Imaging Metrics of a Murine Model of p301L Tau Induced Tauopathy.

机构信息

Basic Sciences, School of Medicine, Loma Linda University, Loma Linda, CA, United States; Neuroscience Graduate Program, University of California, Riverside, CA, United States.

Basic Sciences, School of Medicine, Loma Linda University, Loma Linda, CA, United States.

出版信息

Neuroscience. 2022 Aug 21;498:144-154. doi: 10.1016/j.neuroscience.2022.06.025. Epub 2022 Jun 24.

Abstract

Diffusion Tensor Imaging (DTI) and Manganese Enhanced MRI (MEMRI) are noninvasive tools to characterize neural fiber microstructure and axonal transport. A combination of both may provide novel insights into the progress of neurodegeneration. To investigate the relationship of DTI and MEMRI in white matter of tauopathy, twelve optic nerves of 11-month-old p301L tau mice were imaged and finished with postmortem immunohistochemistry. MEMRI was used to quantify Mn2+ accumulation rates in the optic nerve (ON, termed ONAR) and the Superior Colliculus (SC, termed SCAR), the primary terminal site of ON in mice. We found that both ONAR and SCAR revealed a significant linear correlation with mean diffusion (mD) and radial diffusion (rD) but not with other DTI quantities. Immunohistochemistry findings showed that ONAR, mD, and rD are significantly correlated with the myelin content (Myelin Basic Protein, p < 0.05) but not with the axonal density (SMI-31), tubulin density, or tau aggregates (AT8 staining). In summary, slower axonal transport appeared to have less myelinated axons and thinner remaining axons, associated with reduced rD and mD of in vivo DTI. A combination of in vivo MEMRI and DTI can provide critical information to delineate the progress of white matter deficits in neurodegenerative diseases.

摘要

弥散张量成像(DTI)和锰增强磁共振成像(MEMRI)是非侵入性工具,可用于描述神经纤维的微观结构和轴突运输。两者的结合可能为神经退行性变的进展提供新的见解。为了研究 tau 病白质中 DTI 和 MEMRI 的关系,对 11 个月大的 p301L tau 小鼠的 12 根视神经进行了成像,并进行了死后免疫组织化学分析。MEMRI 用于定量 Mn2+在视神经(ON)中的积累率(称为 ONAR)和上丘(SC)中的积累率(称为 SCAR),ON 在小鼠中的主要末端部位。我们发现,ONAR 和 SCAR 与平均扩散(mD)和径向扩散(rD)均呈显著线性相关,但与其他 DTI 量无关。免疫组织化学结果表明,ONAR、mD 和 rD 与髓鞘含量(髓鞘碱性蛋白,p < 0.05)显著相关,但与轴突密度(SMI-31)、微管蛋白密度或 tau 聚集(AT8 染色)无关。总之,较慢的轴突运输似乎具有较少的髓鞘化轴突和更细的剩余轴突,与体内 DTI 的 rD 和 mD 降低有关。体内 MEMRI 和 DTI 的组合可以提供关键信息,以描绘神经退行性疾病中白质缺陷的进展。

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