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内胚层和血管内皮发育过程中交替启动子区域的差异调控。

Differential regulation of alternate promoter regions in during endodermal and vascular endothelial development.

作者信息

Trinh Linh T, Osipovich Anna B, Sampson Leesa, Wong Jonathan, Wright Chris V E, Magnuson Mark A

机构信息

Department of Cell and Developmental Biology, Vanderbilt University, Nashville, TN 37232, USA.

Center for Stem Cell Biology, Vanderbilt University, Nashville, TN 37232, USA.

出版信息

iScience. 2022 Aug 11;25(9):104905. doi: 10.1016/j.isci.2022.104905. eCollection 2022 Sep 16.

Abstract

gene expression is essential for both endothelial and endodermal cell differentiation. To better understand the genetic basis for the expression of multiple mRNA forms, we identified and performed CRISPR/Cas9 mutagenesis of two evolutionarily conserved promoter regions (CRs). The deletion of the upstream and endothelial cell-specific CR1 caused only a modest increase in lympho-vasculogenesis likely via reduced Notch signaling downstream of SOX17. In contrast, the deletion of the downstream CR2 region, which functions in both endothelial and endodermal cells, impairs both vascular and endodermal development causing death by embryonic day 12.5. Analyses of 3D chromatin looping, transcription factor binding, histone modification, and chromatin accessibility data at the locus and surrounding region further support differential regulation of the two promoters during the development.

摘要

基因表达对于内皮细胞和内胚层细胞的分化都至关重要。为了更好地理解多种mRNA形式表达的遗传基础,我们鉴定并对两个进化上保守的启动子区域(CRs)进行了CRISPR/Cas9诱变。上游内皮细胞特异性CR1的缺失可能通过降低SOX17下游的Notch信号,仅导致淋巴管生成适度增加。相比之下,在内皮细胞和内胚层细胞中均起作用的下游CR2区域的缺失,会损害血管和内胚层发育,导致在胚胎第12.5天死亡。对该基因座及其周围区域的三维染色质环化、转录因子结合、组蛋白修饰和染色质可及性数据的分析进一步支持了在发育过程中两个启动子的差异调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/40a8/9421400/6b351f59fc87/fx1.jpg

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