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首页> 外文期刊>PLoS Biology >Schlemm's Canal Is a Unique Vessel with a Combination of Blood Vascular and Lymphatic Phenotypes that Forms by a Novel Developmental Process
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Schlemm's Canal Is a Unique Vessel with a Combination of Blood Vascular and Lymphatic Phenotypes that Forms by a Novel Developmental Process

机译:Schlemm的运河是一种独特的船只,具有血管和淋巴表表型的组合,这些血管和淋巴表表型通过新颖的发育过程形成

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Schlemm's canal (SC) plays central roles in ocular physiology. These roles depend on the molecular phenotypes of SC endothelial cells (SECs). Both the specific phenotype of SECs and development of SC remain poorly defined. To allow a modern and extensive analysis of SC and its origins, we developed a new whole-mount procedure to visualize its development in the context of surrounding tissues. We then applied genetic lineage tracing, specific-fluorescent reporter genes, immunofluorescence, high-resolution confocal microscopy, and three-dimensional (3D) rendering to study SC. Using these techniques, we show that SECs have a unique phenotype that is a blend of both blood and lymphatic endothelial cell phenotypes. By analyzing whole mounts of postnatal mouse eyes progressively to adulthood, we show that SC develops from blood vessels through a newly discovered process that we name “canalogenesis.” Functional inhibition of KDR (VEGFR2), a critical receptor in initiating angiogenesis, shows that this receptor is required during canalogenesis. Unlike angiogenesis and similar to stages of vasculogenesis, during canalogenesis tip cells divide and form branched chains prior to vessel formation. Differing from both angiogenesis and vasculogenesis, during canalogenesis SECs express Prox1, a master regulator of lymphangiogenesis and lymphatic phenotypes. Thus, SC development resembles a blend of vascular developmental programs. These advances define SC as a unique vessel with a combination of blood vascular and lymphatic phenotypes. They are important for dissecting its functions that are essential for ocular health and normal vision.
机译:Schlemm的运河(SC)在眼部生理学中起着中心作用。这些作用取决于Sc内皮细胞(SEC)的分子表型。 SEC的特定表型和SC的发育都仍然定义不足。为了允许对SC及其起源进行现代和广泛的分析,我们开发了一种新的全部安装程序,以在周围组织的背景下可视化其发展。然后,我们应用遗传谱系追踪,特异性荧光报道基因,免疫荧光,高分辨率共聚焦显微镜,以及三维(3D)渲染研究SC。使用这些技术,我们表明SEC具有独特的表型,这是血液和淋巴内皮细胞表型的混合。通过逐渐分析到成年期的后期鼠标眼睛,我们表明SC通过新发现的过程从血管开发,以至于我们命名为“CANOALOCALE”的过程。 KDR(VEGFR2)的功能抑制,引发血管生成中的关键受体,表明在CaCoO发生期间需要该受体。与血管生成和类似于血管生成的阶段,在CaSalocesis尖端细胞期间分裂并在血管形成之前形成支链。与血管生成和血管生成不同,在Canalogyesis秒Express prox1期间,淋巴管发生和淋巴表表型的母稳压器。因此,SC开发类似于血管发育方案的混合。这些进步将SC定义为具有血管和淋巴表表型组合的独特血管。它们对于解剖其对眼部健康和正常视觉至关重要的功能非常重要。

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