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Insights into the binding of intrinsically disordered proteins from molecular dynamics simulation
Author(s) -
Baker Christopher M.,
Best Robert B.
Publication year - 2013
Publication title -
wiley interdisciplinary reviews: computational molecular science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.126
H-Index - 81
eISSN - 1759-0884
pISSN - 1759-0876
DOI - 10.1002/wcms.1167
Subject(s) - intrinsically disordered proteins , folding (dsp implementation) , flexibility (engineering) , molecular dynamics , computational biology , computer science , nanotechnology , chemistry , biology , biophysics , engineering , mathematics , materials science , computational chemistry , statistics , electrical engineering
Intrinsically disordered proteins ( IDP s) are a class of protein that, in the native state, possess no well‐defined secondary or tertiary structure, existing instead as dynamic ensembles of conformations. They are biologically important, with approximately 20% of all eukaryotic proteins disordered, and found at the heart of many biochemical networks. To fulfil their biological roles, many IDP s need to bind to proteins and/or nucleic acids. And although unstructured in solution, IDP s typically fold into a well‐defined three‐dimensional structure upon interaction with a binding partner. The flexibility and structural diversity inherent to IDP s makes this coupled folding and binding difficult to study at atomic resolution by experiment alone, and computer simulation currently offers perhaps the best opportunity to understand this process. But simulation of coupled folding and binding is itself extremely challenging; these molecules are large and highly flexible, and their binding partners, such as DNA or cyclins, are also often large. Therefore, their study requires either simplified representations, advanced enhanced sampling schemes, or both. It is not always clear that existing simulation techniques, optimized for studying folded proteins, are well suited to IDP s. In this article, we examine the progress that has been made in the study of coupled folding and binding using molecular dynamics simulation. We summarize what has been learnt, and examine the state of the art in terms of both methodologies and models. We also consider the lessons to be learnt from advances in other areas of simulation and highlight the issues that remain of be addressed. This article is categorized under: Molecular and Statistical Mechanics > Molecular Dynamics and Monte-Carlo Methods