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含 RNA 识别基序的人类 RNA 结合蛋白的模块化结构和功能注释。

Modular architecture and functional annotation of human RNA-binding proteins containing RNA recognition motif.

机构信息

School of Bio Science, Indian Institute of Technology Kharagpur, Kharagpur 721302, India; Computational Structural Biology Laboratory, Department of Biotechnology, Indian Institute of Technology Kharagpur, Kharagpur 721302, India.

Computational Structural Biology Laboratory, Department of Biotechnology, Indian Institute of Technology Kharagpur, Kharagpur 721302, India.

出版信息

Biochimie. 2023 Jun;209:116-130. doi: 10.1016/j.biochi.2023.01.017. Epub 2023 Jan 27.

Abstract

RNA-binding proteins (RBPs) are structurally and functionally diverse macromolecules with significant involvement in several post-transcriptional gene regulatory processes and human diseases. RNA recognition motif (RRM) is one of the most abundant RNA-binding domains in human RBPs. The unique modular architecture of each RBP containing RRM is crucial for its diverse target recognition and function. Genome-wide study of these structurally conserved and functionally diverse domains can enhance our understanding of their functional implications. In this study, modular architecture of RRM containing RBPs in human proteome is identified and systematically analysed. We observe that 30% of human RBPs with RNA-binding function contain RRM in single or multiple repeats or with other domains with maximum of six repeats. Zinc-fingers are the most frequently co-occurring domain partner of RRMs. Human RRM containing RBPs mostly belong to RNA metabolism class of proteins and are significantly enriched in two functional pathways including spliceosome and mRNA surveillance. Various human diseases are associated with 18% of the RRM containing RBPs. Single RRM containing RBPs are highly enriched in disorder regions. Gene ontology (GO) molecular functions including poly(A), poly(U) and miRNA binding are highly depleted in RBPs with single RRM, indicating the significance of modular nature of RRMs in specific function. The current study reports all the possible domain architectures of RRM containing human RBPs and their functional enrichment. The idea of domain architecture, and how they confer specificity and new functionalities to RBPs, can help in re-designing of modular RRM containing RBPs with re-engineered function.

摘要

RNA 结合蛋白 (RBPs) 是结构和功能多样化的大分子,在多个转录后基因调控过程和人类疾病中具有重要作用。RNA 识别基序 (RRM) 是人类 RBP 中最丰富的 RNA 结合域之一。每个含有 RRM 的 RBP 的独特模块化结构对于其多样化的靶标识别和功能至关重要。对这些结构保守且功能多样化的结构域进行全基因组研究,可以增强我们对其功能意义的理解。在这项研究中,鉴定并系统分析了人类蛋白质组中含有 RRM 的 RBP 的模块化结构。我们观察到,具有 RNA 结合功能的 30%人类 RBPs 含有一个或多个 RRM 重复或与其他含有最多六个重复的结构域。锌指是 RRM 最常共同出现的结构域伙伴。含有 RRM 的人类 RBP 主要属于 RNA 代谢类蛋白质,并在包括剪接体和 mRNA 监测在内的两个功能途径中显著富集。18%的含有 RRM 的 RBP 与各种人类疾病有关。单个 RRM 含有 RBP 高度富集于无规卷曲区域。GO 分子功能,包括 poly(A)、poly(U)和 miRNA 结合,在含有单个 RRM 的 RBP 中高度缺失,表明 RRM 模块化性质在特定功能中的重要性。本研究报告了含有 RRM 的人类 RBP 的所有可能的结构域架构及其功能富集。结构域架构的概念,以及它们如何赋予 RBP 特异性和新功能,可以帮助重新设计具有重新设计功能的模块化 RRM 含有 RBP。

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