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毛细血管-静脉引流受损会导致衰老过程中小鼠白质中的胶质增生和脱髓鞘。

Impaired capillary-venous drainage contributes to gliosis and demyelination in mouse white matter during aging.

作者信息

Stamenkovic Stefan, Schmid Franca, Gurler Gokce, Abolmaali Farzaneh, Weitermann Nicolas A, Takasaki Kevin T, Bonney Stephanie K, Sosa Maria J, Bennett Hannah C, Kim Yongsoo, Waters Jack, Shih Andy Y

机构信息

Center for Developmental Biology and Regenerative Medicine, Seattle Children's Research Institute, Seattle, WA, USA.

ARTORG Center for Biomedical Engineering Research, University of Bern, Bern, Switzerland.

出版信息

Nat Neurosci. 2025 Aug 12. doi: 10.1038/s41593-025-02023-z.

Abstract

The progressive loss of cerebral white matter during aging contributes to cognitive decline, but whether reduced blood flow is a cause or a consequence remains debatable. Using deep multi-photon imaging in mice, we examined microvascular networks perfusing myelinated tissues in cortical layer 6 and the corpus callosum. We identified sparse, wide-reaching venules, termed principal cortical venules, which exclusively drain deep tissues and resemble the vasculature at the human cortex and U-fiber interface. Aging led to selective constriction and rarefaction of capillaries in deep branches of principal cortical venules. This resulted in mild hypoperfusion that was associated with microgliosis, astrogliosis and demyelination in deep tissues, but not the upper cortex. Induction of comparable hypoperfusion in adult mice using carotid artery stenosis triggered a similar tissue pathology specific to layer 6 and the corpus callosum. Thus, impaired capillary-venous drainage is a contributor to hypoperfusion and a potential therapeutic target for preserving blood flow to white matter during aging.

摘要

衰老过程中脑白质的渐进性丧失会导致认知能力下降,但血流量减少是原因还是结果仍存在争议。我们利用对小鼠进行的深层多光子成像,研究了灌注皮质第6层和胼胝体中髓鞘化组织的微血管网络。我们发现了稀疏且分布广泛的小静脉,称为主要皮质小静脉,它们专门引流深部组织,类似于人类皮质和U形纤维界面处的脉管系统。衰老导致主要皮质小静脉深部分支中的毛细血管选择性收缩和稀疏。这导致了轻度灌注不足,其与深部组织中的小胶质细胞增生、星形胶质细胞增生和脱髓鞘有关,但与上层皮质无关。使用颈动脉狭窄在成年小鼠中诱导类似的灌注不足会引发类似的特定于第6层和胼胝体的组织病理学变化。因此,毛细血管-静脉引流受损是灌注不足的一个原因,也是衰老过程中保留白质血流的一个潜在治疗靶点。

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