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Physics-based modeling provides predictive understanding of selectively promiscuous substrate binding by Hsp70 chaperones

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  • Erik B Nordquist
  • Charles A English
  • Eugenia M Clerico
  • Woody Sherman
  • Lila M Gierasch
  • Jianhan Chen

Abstract

To help cells cope with protein misfolding and aggregation, Hsp70 molecular chaperones selectively bind a variety of sequences (“selective promiscuity”). Statistical analyses from substrate-derived peptide arrays reveal that DnaK, the E. coli Hsp70, binds to sequences containing three to five branched hydrophobic residues, although otherwise the specific amino acids can vary considerably. Several high-resolution structures of the substrate -binding domain (SBD) of DnaK bound to peptides reveal a highly conserved configuration of the bound substrate and further suggest that the substrate-binding cleft consists of five largely independent sites for interaction with five consecutive substrate residues. Importantly, both substrate backbone orientations (N- to C- and C- to N-) allow essentially the same backbone hydrogen-bonding and side-chain interactions with the chaperone. In order to rationalize these observations, we performed atomistic molecular dynamics simulations to sample the interactions of all 20 amino acid side chains in each of the five sites of the chaperone in the context of the conserved substrate backbone configurations. The resulting interaction energetics provide the basis set for deriving a predictive model that we call Paladin (Physics-based model of DnaK-Substrate Binding). Trained using available peptide array data, Paladin can distinguish binders and nonbinders of DnaK with accuracy comparable to existing predictors and further predicts the detailed configuration of the bound sequence. Tested using existing DnaK-peptide structures, Paladin correctly predicted the binding register in 10 out of 13 substrate sequences that bind in the N- to C- orientation, and the binding orientation in 16 out of 22 sequences. The physical basis of the Paladin model provides insight into the origins of how Hsp70s bind substrates with a balance of selectivity and promiscuity. The approach described here can be extended to other Hsp70s where extensive peptide array data is not available.Author summary: Molecular chaperones are proteins that help prevent misfolding and aggregation of their substrates. This is a complex task, as the cell is very crowded, and the chaperone must efficiently bind to misfolded regions of the client protein while avoiding well-folded proteins. An additional confounding detail is that proteins can enter the binding cleft of some Hsp70s in two orientations, a fact often unaccounted for by existing sequence-based models.

Suggested Citation

  • Erik B Nordquist & Charles A English & Eugenia M Clerico & Woody Sherman & Lila M Gierasch & Jianhan Chen, 2021. "Physics-based modeling provides predictive understanding of selectively promiscuous substrate binding by Hsp70 chaperones," PLOS Computational Biology, Public Library of Science, vol. 17(11), pages 1-24, November.
    • Handle: RePEc:plo:pcbi00:1009567
    DOI: 10.1371/journal.pcbi.1009567
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    References listed on IDEAS

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    1. Joost Van Durme & Sebastian Maurer-Stroh & Rodrigo Gallardo & Hannah Wilkinson & Frederic Rousseau & Joost Schymkowitz, 2009. "Accurate Prediction of DnaK-Peptide Binding via Homology Modelling and Experimental Data," PLOS Computational Biology, Public Library of Science, vol. 5(8), pages 1-9, August.
    2. Aliza B Rubenstein & Manasi A Pethe & Sagar D Khare, 2017. "MFPred: Rapid and accurate prediction of protein-peptide recognition multispecificity using self-consistent mean field theory," PLOS Computational Biology, Public Library of Science, vol. 13(6), pages 1-24, June.
    3. F. Ulrich Hartl & Andreas Bracher & Manajit Hayer-Hartl, 2011. "Molecular chaperones in protein folding and proteostasis," Nature, Nature, vol. 475(7356), pages 324-332, July.
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