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Predicting Secondary Structure Propensities in IDPs Using Simple Statistics from Three-Residue Fragments

Intrinsically disordered proteins (IDPs) play key functional roles facilitated by their inherent plasticity. In most of the cases, IDPs recognize their partners through partially structured elements inserted in fully disordered chains. The identification and characterization of these elements is fun...

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Published in:	Journal of molecular biology 2020-09, Vol.432 (19), p.5447-5459
Main Authors:	Estaña, Alejandro, Barozet, Amélie, Mouhand, Assia, Vaisset, Marc, Zanon, Christophe, Fauret, Pierre, Sibille, Nathalie, Bernadó, Pau, Cortés, Juan
Format:	Article
Language:	English
Subjects:	Amino Acid Sequence Animals Biochemistry Biochemistry, Molecular Biology Bioinformatics Biophysics Computer Science Databases, Protein Humans intrinsically disordered proteins Intrinsically Disordered Proteins - chemistry Life Sciences Models, Molecular molecular recognition elements Protein Conformation Protein Structure, Secondary secondary structure prediction short linear motifs Software structural database
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creator	Estaña, Alejandro Barozet, Amélie Mouhand, Assia Vaisset, Marc Zanon, Christophe Fauret, Pierre Sibille, Nathalie Bernadó, Pau Cortés, Juan
description	Intrinsically disordered proteins (IDPs) play key functional roles facilitated by their inherent plasticity. In most of the cases, IDPs recognize their partners through partially structured elements inserted in fully disordered chains. The identification and characterization of these elements is fundamental to understand the functional mechanisms of IDPs. Although several computational methods have been developed to identify order within disordered chains, most of the current secondary structure predictors are focused on globular proteins and are not necessarily appropriate for IDPs. Here, we present a comprehensible method, called Local Structural Propensity Predictor (LS2P), to predict secondary structure elements from IDP sequences. LS2P performs statistical analyses from a database of three-residue fragments extracted from coil regions of high-resolution protein structures. In addition to identifying scarcely populated helical and extended regions, the method pinpoints short stretches triggering β-turn formation or promoting α-helices. The simplicity of the method enables a direct connection between experimental observations and structural features encoded in IDP sequences. [Display omitted] •Partially structured motifs in IDPs are important for function.•LS2P is a new method to predict secondary structures in IDPs from their sequences.•Simple statistical approach using a structural database of three-residue fragments•LS2P connects sequence with structural features and experimental observations.•LS2P is publicly available through a web server.
doi_str_mv	10.1016/j.jmb.2020.07.026
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In most of the cases, IDPs recognize their partners through partially structured elements inserted in fully disordered chains. The identification and characterization of these elements is fundamental to understand the functional mechanisms of IDPs. Although several computational methods have been developed to identify order within disordered chains, most of the current secondary structure predictors are focused on globular proteins and are not necessarily appropriate for IDPs. Here, we present a comprehensible method, called Local Structural Propensity Predictor (LS2P), to predict secondary structure elements from IDP sequences. LS2P performs statistical analyses from a database of three-residue fragments extracted from coil regions of high-resolution protein structures. In addition to identifying scarcely populated helical and extended regions, the method pinpoints short stretches triggering β-turn formation or promoting α-helices. 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In most of the cases, IDPs recognize their partners through partially structured elements inserted in fully disordered chains. The identification and characterization of these elements is fundamental to understand the functional mechanisms of IDPs. Although several computational methods have been developed to identify order within disordered chains, most of the current secondary structure predictors are focused on globular proteins and are not necessarily appropriate for IDPs. Here, we present a comprehensible method, called Local Structural Propensity Predictor (LS2P), to predict secondary structure elements from IDP sequences. LS2P performs statistical analyses from a database of three-residue fragments extracted from coil regions of high-resolution protein structures. In addition to identifying scarcely populated helical and extended regions, the method pinpoints short stretches triggering β-turn formation or promoting α-helices. 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subjects	Amino Acid Sequence Animals Biochemistry Biochemistry, Molecular Biology Bioinformatics Biophysics Computer Science Databases, Protein Humans intrinsically disordered proteins Intrinsically Disordered Proteins - chemistry Life Sciences Models, Molecular molecular recognition elements Protein Conformation Protein Structure, Secondary secondary structure prediction short linear motifs Software structural database
title	Predicting Secondary Structure Propensities in IDPs Using Simple Statistics from Three-Residue Fragments
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