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血管生成星形细胞模板的形成受神经视网膜的调节,这种调节方式依赖于 HIF-1。

The formation of an angiogenic astrocyte template is regulated by the neuroretina in a HIF-1-dependent manner.

机构信息

Department of Cell Differentiation, The Sakaguchi Laboratory, School of Medicine, Keio University, 35 Shinanomachi, Shinjuku-ku, Tokyo 160-8582, Japan.

出版信息

Dev Biol. 2012 Mar 1;363(1):106-14. doi: 10.1016/j.ydbio.2011.12.027. Epub 2011 Dec 24.

DOI:10.1016/j.ydbio.2011.12.027
PMID:22226979
Abstract

The vascular and nervous systems display a high degree of cross-talk and depend on each other functionally. In the vascularization of the central nervous system, astrocytes have been thought to sense tissue oxygen levels in hypoxia-inducible factors (HIFs)-dependent manner and control the vascular growth into the hypoxic area by secreting VEGF. However, recent genetic evidences demonstrate that not only astrocyte HIFs but also astrocyte VEGF expression is dispensable for developmental angiogenesis of the retina. This study demonstrates that hypoxia-inducible factor 1 alpha subunit (HIF-1α), a key transcription factor involved in cellular responses to hypoxia, is most abundantly expressed in the neuroretina, especially retinal progenitor cells (RPCs). A neuroretina-specific knockout of HIF-1α (αCre(+)Hif1α(flox/flox)) showed impaired vascular development characterized by decreased tip cell filopodia and reduced vessel branching. The astrocyte network was hypoplastic in αCre(+)Hif1α(flox/flox) mice. Mechanistically, platelet-derived growth factor A (PDGF-A), a mitogen for astrocytes, was downregulated in the neuroretina of αCre(+)Hif1α(flox/flox) mice. Supplementing PDGF-A restored reduced astrocytic and vascular density in αCre(+)Hif1α(flox/flox) mice. Our data demonstrates that the neuroretina but not astrocytes acts as a primary oxygen sensor which ultimately controls the retinal vascular development by regulating an angiogenic astrocyte template.

摘要

血管系统和神经系统具有高度的相互交流作用,并在功能上相互依赖。在中枢神经系统的血管生成中,星形胶质细胞被认为以缺氧诱导因子 (HIFs) 依赖的方式感知组织中的氧水平,并通过分泌 VEGF 来控制血管向缺氧区域生长。然而,最近的遗传证据表明,不仅星形胶质细胞的 HIFs,而且星形胶质细胞的 VEGF 表达对于视网膜的发育性血管生成都是可有可无的。本研究表明,缺氧诱导因子 1 ɑ 亚基 (HIF-1α),作为细胞对缺氧反应的关键转录因子,在神经视网膜中表达最为丰富,尤其是在视网膜祖细胞 (RPCs) 中。神经视网膜特异性的 HIF-1α 基因敲除 (αCre(+)Hif1α(flox/flox)) 表现出血管发育受损的特征,表现为尖端细胞丝状伪足减少和血管分支减少。αCre(+)Hif1α(flox/flox) 小鼠的星形胶质细胞网络发育不良。在机制上,血小板衍生生长因子 A (PDGF-A),一种星形胶质细胞的有丝分裂原,在 αCre(+)Hif1α(flox/flox) 小鼠的神经视网膜中下调。补充 PDGF-A 可恢复 αCre(+)Hif1α(flox/flox) 小鼠中减少的星形胶质细胞和血管密度。我们的数据表明,神经视网膜而不是星形胶质细胞作为主要的氧传感器,通过调节血管生成星形胶质细胞模板来最终控制视网膜血管发育。

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