在发育和成年小鼠中绘制器官型内皮多样性的转录和表观遗传景观。

IF 9.4 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Manuel E Cantu Gutierrez, Matthew C Hill, Gabrielle E Largoza, William B Gillespie, James F Martin, Joshua D Wythe
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引用次数: 0

摘要

血管内皮在不同的血管类型中具有独特的分子和功能特性,如动脉、静脉和毛细血管之间,以及不同器官之间,如肝脏的渗漏性窦内皮与大脑的不渗透血管。然而,调控内皮器官特化的转录网络仍不清楚。在这里,我们分析了小鼠肝脏、肺、心脏、肾脏、大脑和视网膜在整个发育时期内皮的染色质和转录景观,以确定内皮异质性的潜在转录调节因子。然后,我们确定了在人脑内皮细胞中哪些假设的调节因子是保守的,并使用单细胞转录组学分析,我们确定了在大脑成熟过程中哪些调节网络是活跃的。最后,我们表明,通过这三种方法确定的转录调节因子在分子和功能上对初始内皮细胞进行了重编程。因此,该资源可用于识别控制器官特异性内皮特化的建立和维持的潜在转录调节因子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mapping the transcriptional and epigenetic landscape of organotypic endothelial diversity in the developing and adult mouse.

The vascular endothelium features unique molecular and functional properties across different vessel types, such as between arteries, veins and capillaries, as well as between different organs, such as the leaky sinusoidal endothelium of the liver versus the impermeable vessels of the brain. However, the transcriptional networks governing endothelial organ specialization remain unclear. Here we profile the accessible chromatin and transcriptional landscapes of the endothelium from the mouse liver, lung, heart, kidney, brain and retina, across developmental time, to identify potential transcriptional regulators of endothelial heterogeneity. We then determine which of these putative regulators are conserved in human brain endothelial cells, and using single-cell transcriptomic profiling, we define which regulatory networks are active during brain maturation. Finally, we show that the putative transcriptional regulators identified by these three approaches molecularly and functionally reprogram naive endothelial cells. Thus, this resource can be used to identify potential transcriptional regulators controlling the establishment and maintenance of organ-specific endothelial specialization.

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