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同源二聚化调节 SOX18 转录因子的内皮细胞特异性特征。

Homodimerization regulates an endothelial specific signature of the SOX18 transcription factor.

机构信息

EMBL Australia node in Single Molecule Science and School of Medical Sciences, The University of New South Wales, Sydney, NSW 2031, Australia.

Institute for Molecular Bioscience, The University of Queensland, Brisbane, QLD 4072, Australia.

出版信息

Nucleic Acids Res. 2018 Nov 30;46(21):11381-11395. doi: 10.1093/nar/gky897.

Abstract

During embryogenesis, vascular development relies on a handful of transcription factors that instruct cell fate in a distinct sub-population of the endothelium (1). The SOXF proteins that comprise SOX7, 17 and 18, are molecular switches modulating arterio-venous and lymphatic endothelial differentiation (2,3). Here, we show that, in the SOX-F family, only SOX18 has the ability to switch between a monomeric and a dimeric form. We characterized the SOX18 dimer in binding assays in vitro, and using a split-GFP reporter assay in a zebrafish model system in vivo. We show that SOX18 dimerization is driven by a novel motif located in the vicinity of the C-terminus of the DNA binding region. Insertion of this motif in a SOX7 monomer forced its assembly into a dimer. Genome-wide analysis of SOX18 binding locations on the chromatin revealed enrichment for a SOX dimer binding motif, correlating with genes with a strong endothelial signature. Using a SOX18 small molecule inhibitor that disrupts dimerization, we revealed that dimerization is important for transcription. Overall, we show that dimerization is a specific feature of SOX18 that enables the recruitment of key endothelial transcription factors, and refines the selectivity of the binding to discrete genomic locations assigned to endothelial specific genes.

摘要

在胚胎发生过程中,血管发育依赖于少数转录因子,这些因子在血管内皮的特定亚群中指导细胞命运(1)。SOX7、17 和 18 组成的 SOXF 蛋白是调节动静脉和淋巴管内皮细胞分化的分子开关(2,3)。在这里,我们表明,在 SOX-F 家族中,只有 SOX18 具有在单体和二聚体形式之间切换的能力。我们在体外结合测定中对 SOX18 二聚体进行了表征,并在体内使用斑马鱼模型系统中的分裂 GFP 报告测定进行了研究。我们表明,SOX18 的二聚化是由 DNA 结合区域附近的一个新基序驱动的。将该基序插入 SOX7 单体中会迫使它组装成二聚体。对染色质上 SOX18 结合位置的全基因组分析显示,SOX 二聚体结合基序富集,与具有强烈内皮特征的基因相关。使用一种破坏二聚化的 SOX18 小分子抑制剂,我们揭示了二聚化对于转录很重要。总的来说,我们表明二聚化是 SOX18 的一个特定特征,它能够募集关键的内皮转录因子,并细化了与分配给内皮特定基因的离散基因组位置的结合选择性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1990/6265484/1f1301d0a554/gky897fig1.jpg

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