Designed protein reveals structural determinants of extreme kinetic stability

The design of stable, functional proteins is difficult. Improved design requires a deeper knowledge of the molecular basis for design outcomes and properties. We previously used a bioinformatics and energy function method to design a symmetric superfold protein composed of repeating structural eleme...

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Veröffentlicht in:	Proceedings of the National Academy of Sciences - PNAS 2015-11, Vol.112 (47), p.14605-14610
Hauptverfasser:	Broom, Aron, Ma, S. Martha, Xia, Ke, Rafalia, Hitesh, Trainor, Kyle, Colón, Wilfredo, Gosavi, Shachi, Meiering, Elizabeth M.
Format:	Artikel
Sprache:	eng
Schlagworte:	Binding Sites Bioinformatics Biological Sciences Computer Simulation Design Detergents - pharmacology Experiments Kinetics Ligands Models, Molecular Peptide Hydrolases - metabolism Protein Engineering - methods Protein Folding - drug effects Protein Stability - drug effects Proteins Proteins - chemistry Proteomics Symmetry Thermodynamics Topology
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container_end_page	14610
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container_title	Proceedings of the National Academy of Sciences - PNAS
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creator	Broom, Aron Ma, S. Martha Xia, Ke Rafalia, Hitesh Trainor, Kyle Colón, Wilfredo Gosavi, Shachi Meiering, Elizabeth M.
description	The design of stable, functional proteins is difficult. Improved design requires a deeper knowledge of the molecular basis for design outcomes and properties. We previously used a bioinformatics and energy function method to design a symmetric superfold protein composed of repeating structural elements with multivalent carbohydrate-binding function, called ThreeFoil. This and similar methods have produced a notably high yield of stable proteins. Using a battery of experimental and computational analyses we show that despite its small size and lack of disulfide bonds, ThreeFoil has remarkably high kinetic stability and its folding is specifically chaperoned by carbohydrate binding. It is also extremely stable against thermal and chemical denaturation and proteolytic degradation. We demonstrate that the kinetic stability can be predicted and modeled using absolute contact order (ACO) and long-range order (LRO), as well as coarse-grained simulations; the stability arises from a topology that includes many long-range contacts which create a large and highly cooperative energy barrier for unfolding and folding. Extensive data from proteomic screens and other experiments reveal that a high ACO/LRO is a general feature of proteins with strong resistances to denaturation and degradation. These results provide tractable approaches for predicting resistance and designing proteins with sufficient topological complexity and long-range interactions to accommodate destabilizing functional features as well as withstand chemical and proteolytic challenge.
doi_str_mv	10.1073/pnas.1510748112
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It is also extremely stable against thermal and chemical denaturation and proteolytic degradation. We demonstrate that the kinetic stability can be predicted and modeled using absolute contact order (ACO) and long-range order (LRO), as well as coarse-grained simulations; the stability arises from a topology that includes many long-range contacts which create a large and highly cooperative energy barrier for unfolding and folding. Extensive data from proteomic screens and other experiments reveal that a high ACO/LRO is a general feature of proteins with strong resistances to denaturation and degradation. 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source	MEDLINE; Jstor Complete Legacy; PubMed Central; Alma/SFX Local Collection; Free Full-Text Journals in Chemistry
subjects	Binding Sites Bioinformatics Biological Sciences Computer Simulation Design Detergents - pharmacology Experiments Kinetics Ligands Models, Molecular Peptide Hydrolases - metabolism Protein Engineering - methods Protein Folding - drug effects Protein Stability - drug effects Proteins Proteins - chemistry Proteomics Symmetry Thermodynamics Topology
title	Designed protein reveals structural determinants of extreme kinetic stability
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