Protein flexibility, not disorder, is intrinsic to molecular recognition.

F1000 Biol Rep

Institut de Biochimie et Biophysique Moléculaire et Cellulaire, Université Paris-Sud 91405-Orsay, France.

Published: January 2013

An 'intrinsically disordered protein' (IDP) is assumed to be unfolded in the cell and perform its biological function in that state. We contend that most intrinsically disordered proteins are in fact proteins waiting for a partner (PWPs), parts of a multi-component complex that do not fold correctly in the absence of other components. Flexibility, not disorder, is an intrinsic property of proteins, exemplified by X-ray structures of many enzymes and protein-protein complexes. Disorder is often observed with purified proteins in vitro and sometimes also in crystals, where it is difficult to distinguish from flexibility. In the crowded environment of the cell, disorder is not compatible with the known mechanisms of protein-protein recognition, and, foremost, with its specificity. The self-assembly of multi-component complexes may, nevertheless, involve the specific recognition of nascent polypeptide chains that are incompletely folded, but then disorder is transient, and it must remain under the control of molecular chaperones and of the quality control apparatus that obviates the toxic effects it can have on the cell.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3542771PMC
http://dx.doi.org/10.3410/B5-2DOI Listing

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