Literature DB >> 23963781

Protein domain definition should allow for conditional disorder.

Kavestri Yegambaram1, Esther M M Bulloch, Richard L Kingston.   

Abstract

Proteins are often classified in a binary fashion as either structured or disordered. However this approach has several deficits. Firstly, protein folding is always conditional on the physiochemical environment. A protein which is structured in some circumstances will be disordered in others. Secondly, it hides a fundamental asymmetry in behavior. While all structured proteins can be unfolded through a change in environment, not all disordered proteins have the capacity for folding. Failure to accommodate these complexities confuses the definition of both protein structural domains and intrinsically disordered regions. We illustrate these points with an experimental study of a family of small binding domains, drawn from the RNA polymerase of mumps virus and its closest relatives. Assessed at face value the domains fall on a structural continuum, with folded, partially folded, and near unstructured members. Yet the disorder present in the family is conditional, and these closely related polypeptides can access the same folded state under appropriate conditions. Any heuristic definition of the protein domain emphasizing conformational stability divides this domain family in two, in a way that makes no biological sense. Structural domains would be better defined by their ability to adopt a specific tertiary structure: a structure that may or may not be realized, dependent on the circumstances. This explicitly allows for the conditional nature of protein folding, and more clearly demarcates structural domains from intrinsically disordered regions that may function without folding.
© 2013 The Protein Society.

Entities:  

Keywords:  RNA-dependent RNA polymerase; coupled binding and folding; intrinsic protein disorder; mumps virus; protein stability; rubulaviruses; stabilizing osmolytes; trimethylamine N-oxide

Mesh:

Substances:

Year:  2013        PMID: 23963781      PMCID: PMC3831666          DOI: 10.1002/pro.2336

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


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