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在人类蛋白质网络中识别出的生物相互作用单元揭示了组织功能的多样化及其对疾病的影响。

Biological interacting units identified in human protein networks reveal tissue-functional diversification and its impact on disease.

作者信息

García-Vaquero Marina L, Gama-Carvalho Margarida, Pinto Francisco R, De Las Rivas Javier

机构信息

University of Lisboa, Faculty of Sciences, BioISI - Biosystems & Integrative Sciences Institute, Campo Grande, C8 bdg, Lisboa 1749-016, Portugal.

Cancer Research Center (CiC-IBMCC, CSIC/USAL and IBSAL), Consejo Superior de Investigaciones Científicas (CSIC), University of Salamanca (USAL) and Instituto de Investigación Biomédica de Salamanca (IBSAL), Salamanca 37007, Spain.

出版信息

Comput Struct Biotechnol J. 2022 Jul 15;20:3764-3778. doi: 10.1016/j.csbj.2022.07.006. eCollection 2022.

Abstract

Protein-protein interactions (PPI) play an essential role in the biological processes that occur in the cell. Therefore, the dissection of PPI networks becomes decisive to model functional coordination and predict pathological de-regulation. Cellular networks are dynamic and proteins display varying roles depending on the tissue-interactomic context. Thus, the use of centrality measures in individual proteins fall short to dissect the functional properties of the cell. For this reason, there is a need for more comprehensive, relational, and context-specific ways to analyze the multiple actions of proteins in different cells and identify specific functional assemblies within global biomolecular networks. Under this framework, we define (BioInt-U) as groups of proteins that interact physically and are enriched in a common Gene Ontology. A search strategy was applied on 33 tissue-specific (TS) PPI networks to generate libraries associated with each particular human tissue. The cross-tissue comparison showed that housekeeping assemblies incorporate different proteins and exhibit distinct network properties depending on the tissue. Furthermore, disease genes (DGs) of tissue-associated pathologies preferentially accumulate in units in the expected tissues, which in turn were more central in the TS networks. Overall, the study reveals a tissue-specific functional diversification based on the identification of specific protein units and suggests vulnerabilities specific of each tissue network, which can be applied to refine protein-disease association methods.

摘要

蛋白质-蛋白质相互作用(PPI)在细胞内发生的生物过程中起着至关重要的作用。因此,剖析PPI网络对于构建功能协调模型和预测病理失调具有决定性意义。细胞网络是动态的,蛋白质根据组织相互作用组学背景发挥不同的作用。因此,使用单个蛋白质的中心性度量不足以剖析细胞的功能特性。出于这个原因,需要更全面、相关且特定于上下文的方法来分析蛋白质在不同细胞中的多种作用,并识别全球生物分子网络中的特定功能组件。在此框架下,我们将(BioInt-U)定义为物理相互作用且在共同基因本体中富集的蛋白质组。我们对33个组织特异性(TS)PPI网络应用了一种搜索策略,以生成与每个特定人类组织相关的文库。跨组织比较表明,管家组件包含不同的蛋白质,并根据组织表现出不同的网络特性。此外,组织相关病理学的疾病基因(DGs)优先在预期组织的单元中积累,而这些单元在TS网络中又更为核心。总体而言,该研究基于特定蛋白质单元的识别揭示了一种组织特异性功能多样化,并提出了每个组织网络特有的脆弱性,可用于完善蛋白质-疾病关联方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d75b/9304429/8cf9fe4963b4/ga1.jpg

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