颅骨祖细胞驱动的脑膜淋巴修复可改善颅缝闭合症的神经认知功能。

Cell stem cell Pub Date : 2023-11-02 Epub Date: 2023-10-19 DOI:10.1016/j.stem.2023.09.012
Li Ma, Qing Chang, Fei Pei, Mengmeng Liu, Wei Zhang, Young-Kwon Hong, Yang Chai, Jian-Fu Chen
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引用次数: 0

摘要

脑膜位于颅骨和大脑之间的界面,含有淋巴血管系统和颅骨祖细胞(SPC)。头骨和大脑是如何交流的在很大程度上仍然未知。我们发现,脑膜淋巴管和脑灌注受损导致Twist1+/-小鼠的神经认知缺陷,Twist1++-小鼠是一种再现人类Saethre-Chotzen综合征的颅缝闭合症动物模型。SPCs的缺失会导致颅骨畸形和颅内压升高(ICP),而将SPCs移植回突变小鼠体内通过两种机制减轻淋巴和大脑缺陷:(1)通过颅骨矫正降低升高的ICP;(2)通过SPC分泌的血管内皮生长因子-C(VEGF-C)促进淋巴内皮细胞(LECs)的生长和迁移。用VEGF-C治疗Twist1+/-小鼠可促进脑膜淋巴管生长,挽救ICP、脑灌注和神经认知功能的缺陷。因此,颅骨通过脑膜淋巴管与大脑功能整合,脑膜淋巴管在颅缝闭合中受损,可以通过VEGF-C通过SPC驱动的淋巴激活来恢复。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Skull progenitor cell-driven meningeal lymphatic restoration improves neurocognitive functions in craniosynostosis.

The meninges lie in the interface between the skull and brain, harboring lymphatic vasculature and skull progenitor cells (SPCs). How the skull and brain communicate remains largely unknown. We found that impaired meningeal lymphatics and brain perfusion drive neurocognitive defects in Twist1+/- mice, an animal model of craniosynostosis recapitulating human Saethre-Chotzen syndrome. Loss of SPCs leads to skull deformities and elevated intracranial pressure (ICP), whereas transplanting SPCs back into mutant mice mitigates lymphatic and brain defects through two mechanisms: (1) decreasing elevated ICP by skull correction and (2) promoting the growth and migration of lymphatic endothelial cells (LECs) via SPC-secreted vascular endothelial growth factor-C (VEGF-C). Treating Twist1+/- mice with VEGF-C promotes meningeal lymphatic growth and rescues defects in ICP, brain perfusion, and neurocognitive functions. Thus, the skull functionally integrates with the brain via meningeal lymphatics, which is impaired in craniosynostosis and can be restored by SPC-driven lymphatic activation via VEGF-C.

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