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紧密连接蛋白闭合蛋白的基因表达包括可变剪接和可变启动子使用。

Gene expression of the tight junction protein occludin includes differential splicing and alternative promoter usage.

作者信息

Mankertz Joachim, Waller Jörg Stefan, Hillenbrand Bernd, Tavalali Shida, Florian Peter, Schöneberg Torsten, Fromm Michael, Schulzke Jörg Dieter

机构信息

Medizinische Klinik I Gastroenterologie, Infektiologie und Rheumatologie, Universitätsklinikum Benjamin Franklin, Freie Universität Berlin, Hindenburgdamm 30, 12000 Berlin, Germany.

出版信息

Biochem Biophys Res Commun. 2002 Nov 15;298(5):657-66. doi: 10.1016/s0006-291x(02)02487-7.

Abstract

Occludin is an integral membrane protein located at the tight junctions of epithelial cells. Multiple domains of occludin are involved in the regulation of paracellular permeability as well as in the targeting of the protein to the tight junction. In this study, different occludin variants were identified on the mRNA level. Four differentially spliced occludin-specific mRNA transcripts were detected. Expression of the resulting proteins revealed an altered subcellular distribution and a loss of co-localization with zonula occludens protein ZO-1 in the tight junction for two of the four splice variants. Our findings demonstrate that the fourth transmembrane domain of occludin is important for targeting occludin to the tight junction. Loss of the fourth transmembrane domain leads to a relocation of the C-terminal domain to the extracellular space. The structural diversity of natural occludin variants is further increased by an additional promoter and transcription start giving rise to an alternative exon 1. Gene expression mediated by this promoter is influenced by the pro-inflammatory cytokine tumor necrosis factor alpha.

摘要

闭合蛋白是一种位于上皮细胞紧密连接处的整合膜蛋白。闭合蛋白的多个结构域参与细胞旁通透性的调节以及该蛋白靶向紧密连接的过程。在本研究中,在mRNA水平上鉴定出了不同的闭合蛋白变体。检测到了四种差异剪接的闭合蛋白特异性mRNA转录本。对所产生蛋白质的表达分析显示,四种剪接变体中的两种在紧密连接处的亚细胞分布发生改变,并且与紧密连接蛋白ZO-1的共定位丧失。我们的研究结果表明,闭合蛋白的第四个跨膜结构域对于将闭合蛋白靶向紧密连接很重要。第四个跨膜结构域的缺失导致C末端结构域重新定位到细胞外空间。另外一个启动子和转录起始位点进一步增加了天然闭合蛋白变体的结构多样性,从而产生了一个替代外显子1。由该启动子介导的基因表达受促炎细胞因子肿瘤坏死因子α的影响。

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