Side-chain interactions form late and cooperatively in the binding reaction between disordered peptides and PDZ domains

S Raza Haq; Celestine N Chi; Anders Bach; Jakob Dogan; Åke Engström; Greta Hultqvist; O. Andreas Karlsson; Patrik Lundström; Linda Celeste Montemiglio; Kristian Strømgaard; Stefano Gianni; Per Jemth

doi:10.1021/ja209341w

Side-chain interactions form late and cooperatively in the binding reaction between disordered peptides and PDZ domains

S Raza Haq, Celestine N Chi, Anders Bach, Jakob Dogan, Åke Engström, Greta Hultqvist, O. Andreas Karlsson, Patrik Lundström, Linda Celeste Montemiglio, Kristian Strømgaard, Stefano Gianni, Per Jemth

31 Citationer (Scopus)

Abstract

Intrinsically disordered proteins are very common and mediate numerous protein-protein and protein-DNA interactions. While it is clear that these interactions are instrumental for the life of the mammalian cell, there is a paucity of data regarding their molecular binding mechanisms. Here we have used short peptides as a model system for intrinsically disordered proteins. Linear free energy relationships based on rate and equilibrium constants for the binding of these peptides to ordered target proteins, PDZ domains, demonstrate that native side-chain interactions form mainly after the rate-limiting barrier for binding and in a cooperative fashion. This finding suggests that these disordered peptides first form a weak encounter complex with non-native interactions. The data do not support the recent notion that the affinities of intrinsically disordered proteins toward their targets are generally governed by their association rate constants. Instead, we observed the opposite for peptide-PDZ interactions, namely, that changes in K _d correlate with changes in k _off.

Originalsprog	Engelsk
Tidsskrift	Journal of the American Chemical Society
Vol/bind	134
Udgave nummer	1
Sider (fra-til)	599-605
ISSN	0002-7863
DOI	https://doi.org/10.1021/ja209341w
Status	Udgivet - 11 jan. 2012

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Haq, S. R., Chi, C. N., Bach, A., Dogan, J., Engström, Å., Hultqvist, G., Karlsson, O. A., Lundström, P., Montemiglio, L. C., Strømgaard, K., Gianni, S., & Jemth, P. (2012). Side-chain interactions form late and cooperatively in the binding reaction between disordered peptides and PDZ domains. Journal of the American Chemical Society, 134(1), 599-605. https://doi.org/10.1021/ja209341w

Haq, SR, Chi, CN, Bach, A, Dogan, J, Engström, Å, Hultqvist, G, Karlsson, OA, Lundström, P, Montemiglio, LC, Strømgaard, K, Gianni, S & Jemth, P 2012, 'Side-chain interactions form late and cooperatively in the binding reaction between disordered peptides and PDZ domains', Journal of the American Chemical Society, bind 134, nr. 1, s. 599-605. https://doi.org/10.1021/ja209341w

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abstract = "Intrinsically disordered proteins are very common and mediate numerous protein-protein and protein-DNA interactions. While it is clear that these interactions are instrumental for the life of the mammalian cell, there is a paucity of data regarding their molecular binding mechanisms. Here we have used short peptides as a model system for intrinsically disordered proteins. Linear free energy relationships based on rate and equilibrium constants for the binding of these peptides to ordered target proteins, PDZ domains, demonstrate that native side-chain interactions form mainly after the rate-limiting barrier for binding and in a cooperative fashion. This finding suggests that these disordered peptides first form a weak encounter complex with non-native interactions. The data do not support the recent notion that the affinities of intrinsically disordered proteins toward their targets are generally governed by their association rate constants. Instead, we observed the opposite for peptide-PDZ interactions, namely, that changes in K d correlate with changes in k off.",

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doi = "10.1021/ja209341w",

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AU - Haq, S Raza

AU - Chi, Celestine N

AU - Bach, Anders

AU - Dogan, Jakob

AU - Engström, Åke

AU - Hultqvist, Greta

AU - Karlsson, O. Andreas

AU - Lundström, Patrik

AU - Montemiglio, Linda Celeste

AU - Strømgaard, Kristian

AU - Gianni, Stefano

AU - Jemth, Per

PY - 2012/1/11

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N2 - Intrinsically disordered proteins are very common and mediate numerous protein-protein and protein-DNA interactions. While it is clear that these interactions are instrumental for the life of the mammalian cell, there is a paucity of data regarding their molecular binding mechanisms. Here we have used short peptides as a model system for intrinsically disordered proteins. Linear free energy relationships based on rate and equilibrium constants for the binding of these peptides to ordered target proteins, PDZ domains, demonstrate that native side-chain interactions form mainly after the rate-limiting barrier for binding and in a cooperative fashion. This finding suggests that these disordered peptides first form a weak encounter complex with non-native interactions. The data do not support the recent notion that the affinities of intrinsically disordered proteins toward their targets are generally governed by their association rate constants. Instead, we observed the opposite for peptide-PDZ interactions, namely, that changes in K d correlate with changes in k off.

AB - Intrinsically disordered proteins are very common and mediate numerous protein-protein and protein-DNA interactions. While it is clear that these interactions are instrumental for the life of the mammalian cell, there is a paucity of data regarding their molecular binding mechanisms. Here we have used short peptides as a model system for intrinsically disordered proteins. Linear free energy relationships based on rate and equilibrium constants for the binding of these peptides to ordered target proteins, PDZ domains, demonstrate that native side-chain interactions form mainly after the rate-limiting barrier for binding and in a cooperative fashion. This finding suggests that these disordered peptides first form a weak encounter complex with non-native interactions. The data do not support the recent notion that the affinities of intrinsically disordered proteins toward their targets are generally governed by their association rate constants. Instead, we observed the opposite for peptide-PDZ interactions, namely, that changes in K d correlate with changes in k off.

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Side-chain interactions form late and cooperatively in the binding reaction between disordered peptides and PDZ domains

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