Binding without folding – the biomolecular function of disordered polyelectrolyte complexes

Benjamin Schuler; Alessandro Borgia; Madeleine B. Borgia; Pétur O. Heidarsson; Erik D. Holmstrom; Daniel Nettels; Andrea Sottini

doi:10.1016/j.sbi.2019.12.006

Binding without folding – the biomolecular function of disordered polyelectrolyte complexes

Benjamin Schuler, Alessandro Borgia, Madeleine B. Borgia, Pétur O. Heidarsson, Erik D. Holmstrom, Daniel Nettels, Andrea Sottini

Faculty of Physical Sciences

University of Iceland

Research output: Contribution to journal › Review article › peer-review

Abstract

Recent evidence shows that oppositely charged intrinsically disordered proteins (IDPs) can form high-affinity complexes that involve neither the formation of secondary or tertiary structure nor site-specific interactions between individual residues. Similar electrostatically dominated interactions have also been identified for positively charged IDPs binding to nucleic acids. These highly disordered polyelectrolyte complexes constitute an extreme case within the spectrum of biomolecular interactions involving disorder. Such interactions are likely to be widespread, since sequence analysis predicts proteins with highly charged disordered regions to be surprisingly numerous. Here, we summarize the insights that have emerged from the highly disordered polyelectrolyte complexes identified so far, and we highlight recent developments and future challenges in (i) establishing models for the underlying highly dynamic structural ensembles, (ii) understanding the novel binding mechanisms associated with them, and (iii) identifying the functional consequences.

Original language	English
Pages (from-to)	66-76
Number of pages	11
Journal	Current Opinion in Structural Biology
Volume	60
DOIs	https://doi.org/10.1016/j.sbi.2019.12.006
Publication status	Published - Feb 2020

Bibliographical note

Funding Information: We thank Robert Best, Katrine Bugge, Aritra Chowdhury, Kingshuk Ghosh, Birthe Kragelund, Davide Mercadante, and Dave Thirumalai for fruitful discussions and comments, and the Swiss National Science Foundation for funding. Publisher Copyright: © 2019 Elsevier Ltd

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title = "Binding without folding – the biomolecular function of disordered polyelectrolyte complexes",

abstract = "Recent evidence shows that oppositely charged intrinsically disordered proteins (IDPs) can form high-affinity complexes that involve neither the formation of secondary or tertiary structure nor site-specific interactions between individual residues. Similar electrostatically dominated interactions have also been identified for positively charged IDPs binding to nucleic acids. These highly disordered polyelectrolyte complexes constitute an extreme case within the spectrum of biomolecular interactions involving disorder. Such interactions are likely to be widespread, since sequence analysis predicts proteins with highly charged disordered regions to be surprisingly numerous. Here, we summarize the insights that have emerged from the highly disordered polyelectrolyte complexes identified so far, and we highlight recent developments and future challenges in (i) establishing models for the underlying highly dynamic structural ensembles, (ii) understanding the novel binding mechanisms associated with them, and (iii) identifying the functional consequences.",

author = "Benjamin Schuler and Alessandro Borgia and Borgia, \{Madeleine B.\} and Heidarsson, \{P{\'e}tur O.\} and Holmstrom, \{Erik D.\} and Daniel Nettels and Andrea Sottini",

note = "Funding Information: We thank Robert Best, Katrine Bugge, Aritra Chowdhury, Kingshuk Ghosh, Birthe Kragelund, Davide Mercadante, and Dave Thirumalai for fruitful discussions and comments, and the Swiss National Science Foundation for funding. Publisher Copyright: {\textcopyright} 2019 Elsevier Ltd",

year = "2020",

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doi = "10.1016/j.sbi.2019.12.006",

language = "English",

volume = "60",

pages = "66--76",

journal = "Current Opinion in Structural Biology",

issn = "0959-440X",

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T1 - Binding without folding – the biomolecular function of disordered polyelectrolyte complexes

AU - Schuler, Benjamin

AU - Borgia, Alessandro

AU - Borgia, Madeleine B.

AU - Heidarsson, Pétur O.

AU - Holmstrom, Erik D.

AU - Nettels, Daniel

AU - Sottini, Andrea

N1 - Funding Information: We thank Robert Best, Katrine Bugge, Aritra Chowdhury, Kingshuk Ghosh, Birthe Kragelund, Davide Mercadante, and Dave Thirumalai for fruitful discussions and comments, and the Swiss National Science Foundation for funding. Publisher Copyright: © 2019 Elsevier Ltd

PY - 2020/2

Y1 - 2020/2

N2 - Recent evidence shows that oppositely charged intrinsically disordered proteins (IDPs) can form high-affinity complexes that involve neither the formation of secondary or tertiary structure nor site-specific interactions between individual residues. Similar electrostatically dominated interactions have also been identified for positively charged IDPs binding to nucleic acids. These highly disordered polyelectrolyte complexes constitute an extreme case within the spectrum of biomolecular interactions involving disorder. Such interactions are likely to be widespread, since sequence analysis predicts proteins with highly charged disordered regions to be surprisingly numerous. Here, we summarize the insights that have emerged from the highly disordered polyelectrolyte complexes identified so far, and we highlight recent developments and future challenges in (i) establishing models for the underlying highly dynamic structural ensembles, (ii) understanding the novel binding mechanisms associated with them, and (iii) identifying the functional consequences.

AB - Recent evidence shows that oppositely charged intrinsically disordered proteins (IDPs) can form high-affinity complexes that involve neither the formation of secondary or tertiary structure nor site-specific interactions between individual residues. Similar electrostatically dominated interactions have also been identified for positively charged IDPs binding to nucleic acids. These highly disordered polyelectrolyte complexes constitute an extreme case within the spectrum of biomolecular interactions involving disorder. Such interactions are likely to be widespread, since sequence analysis predicts proteins with highly charged disordered regions to be surprisingly numerous. Here, we summarize the insights that have emerged from the highly disordered polyelectrolyte complexes identified so far, and we highlight recent developments and future challenges in (i) establishing models for the underlying highly dynamic structural ensembles, (ii) understanding the novel binding mechanisms associated with them, and (iii) identifying the functional consequences.

UR - https://www.scopus.com/pages/publications/85076695662

U2 - 10.1016/j.sbi.2019.12.006

DO - 10.1016/j.sbi.2019.12.006

M3 - Review article

C2 - 31874413

SN - 0959-440X

VL - 60

SP - 66

EP - 76

JO - Current Opinion in Structural Biology

JF - Current Opinion in Structural Biology

ER -

Binding without folding – the biomolecular function of disordered polyelectrolyte complexes

Abstract

Bibliographical note

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