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人类蛋白质组中不同类型的紊乱:选择性剪接的功能意义。

Distinct types of disorder in the human proteome: functional implications for alternative splicing.

机构信息

The Donnelly Centre, University of Toronto, Toronto, Ontario, Canada.

出版信息

PLoS Comput Biol. 2013 Apr;9(4):e1003030. doi: 10.1371/journal.pcbi.1003030. Epub 2013 Apr 25.

Abstract

Intrinsically disordered regions have been associated with various cellular processes and are implicated in several human diseases, but their exact roles remain unclear. We previously defined two classes of conserved disordered regions in budding yeast, referred to as "flexible" and "constrained" conserved disorder. In flexible disorder, the property of disorder has been positionally conserved during evolution, whereas in constrained disorder, both the amino acid sequence and the property of disorder have been conserved. Here, we show that flexible and constrained disorder are widespread in the human proteome, and are particularly common in proteins with regulatory functions. Both classes of disordered sequences are highly enriched in regions of proteins that undergo tissue-specific (TS) alternative splicing (AS), but not in regions of proteins that undergo general (i.e., not tissue-regulated) AS. Flexible disorder is more highly enriched in TS alternative exons, whereas constrained disorder is more highly enriched in exons that flank TS alternative exons. These latter regions are also significantly more enriched in potential phosphosites and other short linear motifs associated with cell signaling. We further show that cancer driver mutations are significantly enriched in regions of proteins associated with TS and general AS. Collectively, our results point to distinct roles for TS alternative exons and flanking exons in the dynamic regulation of protein interaction networks in response to signaling activity, and they further suggest that alternatively spliced regions of proteins are often functionally altered by mutations responsible for cancer.

摘要

无规则区域与各种细胞过程相关联,并与几种人类疾病有关,但它们的确切作用仍不清楚。我们之前在芽殖酵母中定义了两类保守的无规则区域,分别称为“灵活”和“约束”保守无规则。在灵活的无序中,无序的性质在进化过程中是位置保守的,而在约束的无序中,氨基酸序列和无序的性质都是保守的。在这里,我们表明灵活和约束的无序在人类蛋白质组中广泛存在,并且在具有调节功能的蛋白质中尤为常见。这两类无序序列在经历组织特异性(TS)可变剪接(AS)的蛋白质区域中高度富集,但在经历一般(即不受组织调节)AS 的蛋白质区域中不富集。灵活的无序在 TS 可变外显子中高度富集,而约束的无序在外显子中高度富集,这些外显子侧翼 TS 可变外显子。这些区域还显著富含与细胞信号转导相关的潜在磷酸化位点和其他短线性基序。我们进一步表明,癌症驱动突变在与 TS 和一般 AS 相关的蛋白质区域中显著富集。总的来说,我们的结果表明,TS 可变外显子和侧翼外显子在响应信号活性的蛋白质相互作用网络的动态调节中具有不同的作用,并且它们进一步表明,负责癌症的突变经常改变蛋白质的可变剪接区域的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7a38/3635989/f825231c81e2/pcbi.1003030.g001.jpg

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