Literature DB >> 28597295

Evolution of intrinsic disorder in eukaryotic proteins.

Joseph B Ahrens1, Janelle Nunez-Castilla1, Jessica Siltberg-Liberles2.   

Abstract

Conformational flexibility conferred though regions of intrinsic structural disorder allows proteins to behave as dynamic molecules. While it is well-known that intrinsically disordered regions can undergo disorder-to-order transitions in real-time as part of their function, we also are beginning to learn more about the dynamics of disorder-to-order transitions along evolutionary time-scales. Intrinsically disordered regions endow proteins with functional promiscuity, which is further enhanced by the ability of some of these regions to undergo real-time disorder-to-order transitions. Disorder content affects gene retention after whole genome duplication, but it is not necessarily conserved. Altered patterns of disorder resulting from evolutionary disorder-to-order transitions indicate that disorder evolves to modify function through refining stability, regulation, and interactions. Here, we review the evolution of intrinsically disordered regions in eukaryotic proteins. We discuss the interplay between secondary structure and disorder on evolutionary time-scales, the importance of disorder for eukaryotic proteome expansion and functional divergence, and the evolutionary dynamics of disorder.

Entities:  

Keywords:  Disorder-to-order transition; Dosage; Evolutionary dynamics; Functional divergence; Gene duplication; Intrinsic disorder; Neutrality; Protein evolution

Mesh:

Substances:

Year:  2017        PMID: 28597295     DOI: 10.1007/s00018-017-2559-0

Source DB:  PubMed          Journal:  Cell Mol Life Sci        ISSN: 1420-682X            Impact factor:   9.261


  111 in total

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8.  Evolution of disorder in Mediator complex and its functional relevance.

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  21 in total

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8.  Proteins of generalist and specialist pathogens differ in their amino acid composition.

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9.  Large-Scale Analyses of Site-Specific Evolutionary Rates across Eukaryote Proteomes Reveal Confounding Interactions between Intrinsic Disorder, Secondary Structure, and Functional Domains.

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