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POU2F1 的结构方面,考虑到功能注释和序列-结构模式。

Structural facets of POU2F1 in light of the functional annotations and sequence-structure patterns.

机构信息

Computer Science and Engineering, Jadavpur University, Kolkata, West Bengal, India.

Federal Research Center "Pushchino Scientific Center for Biological Research of the Russian Academy of Sciences", Institute for Biological Instrumentation of the Russian Academy of Sciences, Pushchino, Moscow Region, Russia.

出版信息

J Biomol Struct Dyn. 2021 Feb;39(3):1093-1105. doi: 10.1080/07391102.2020.1733092. Epub 2020 Mar 2.

Abstract

POU domain class 2 homebox 1 or POU2F1 is broadly known as an important transcription factor. Due to its association with different types of malignancies, POU2F1 became one of the key factors in pancancer analysis. However, in spite of considering this protein as a potential drug target, none of the drug targeting POU2F1 has been designed as of yet due to the extreme structural flexibility of this protein. In this article, we have proposed a three-level comprehensive framework for understanding the structural conservation and co-variation of POU2F1. First, a gene regulatory network based on the normal and pathological functions of POU2F1 has been created for better understanding the strong association between POU2F1 deregulation and cancers. After that, based on the evolutionary sequence space analysis, the comparative sequence dynamics of the protein members of POU domain family has been studied mostly between non-human and human species. Subsequently, the reciprocity effect of the residual co-variation has been identified through direct coupling analysis. Along with that, the structure of POU2F1 has been analyzed depending on quality assessment and normal mode-based structure network. Comparing the sequence and structure space information, the most significant set of residues viz., 3, 9, 13, 17, 20, 21, 28, 35, and 36 have been identified as structural facet for function. This study demonstrates that the structural malleability of POU2F1 serves as one of the prime reason behind its functional multiplicity in terms of protein moonlighting. Communicated by Ramaswamy H. Sarma.

摘要

POU 结构域类 2 同源框 1 或 POU2F1 通常被认为是一种重要的转录因子。由于其与多种恶性肿瘤有关,POU2F1 成为泛癌分析的关键因素之一。然而,尽管考虑将这种蛋白质作为潜在的药物靶点,但由于该蛋白质的结构极其灵活,目前尚未设计针对 POU2F1 的药物。在本文中,我们提出了一个三级综合框架,用于理解 POU2F1 的结构保守性和共变。首先,基于 POU2F1 的正常和病理功能创建了一个基因调控网络,以更好地理解 POU2F1 失调与癌症之间的强关联。之后,基于进化序列空间分析,研究了 POU 结构域家族蛋白成员之间在非人类和人类物种之间的比较序列动力学。随后,通过直接耦合分析确定了剩余共变的相互作用效应。同时,根据质量评估和基于正常模式的结构网络分析了 POU2F1 的结构。比较序列和结构空间信息,确定了最重要的一组残基 3、9、13、17、20、21、28、35 和 36 作为结构功能面。这项研究表明,POU2F1 的结构可塑性是其在蛋白质 moonlighting 方面具有多功能性的主要原因之一。由 Ramaswamy H. Sarma 传达。

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