| Literature DB >> 33712886 |
Chang-Xiong Gong1, Qin Zhang1, Xiao-Yi Xiong1, Jun-Jie Yuan1, Guo-Qiang Yang1, Jia-Cheng Huang1, Juan Liu1, Chun-Mei Duan1, Zhong-Ming Qiu1, Zhao-You Meng1, Kai Zhou1, Fa-Xiang Wang1, Chen-Hao Zhao1, Fangfei Li2, Qing-Wu Yang3.
Abstract
Neurons in the penumbra (the area surrounding ischemic tissue that consists of still viable tissue but with reduced blood flow and oxygen transport) may be rescued following stroke if adequate perfusion is restored in time. It has been speculated that post-stroke angiogenesis in the penumbra can reduce damage caused by ischemia. However, the mechanism for neovasculature formation in the brain remains unclear and vascular-targeted therapies for brain ischemia remain suboptimal. Here, we show that VEGFR1 was highly upregulated in pericytes after stroke. Knockdown of VEGFR1 in pericytes led to increased infarct area and compromised post-ischemia vessel formation. Furthermore, in vitro studies confirmed a critical role for pericyte-derived VEGFR1 in both endothelial tube formation and pericyte migration. Interestingly, our results show that pericyte-derived VEGFR1 has opposite effects on Akt activity in endothelial cells and pericytes. Collectively, these results indicate that pericyte-specific expression of VEGFR1 modulates ischemia-induced vessel formation and vascular integrity in the brain.Entities:
Keywords: Cerebrovascular; Ischemia; Pericyte; Stroke; VEGFR1
Mesh:
Year: 2021 PMID: 33712886 DOI: 10.1007/s10571-021-01071-w
Source DB: PubMed Journal: Cell Mol Neurobiol ISSN: 0272-4340 Impact factor: 5.046