Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain

Stapled peptides are promising protein–protein interaction (PPI) inhibitors that can increase the binding potency. Different from small-molecule inhibitors in which the binding mainly depends on energetic interactions with their protein targets, the binding of stapled peptides has long been suggeste...

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Autores principales: Unarta, Ilona Christy, Xu, Jianchao, Shang, Yuan, Cheung, Carina Hey Pui, Zhu, Ruichi, Chen, Xudong, Cao, Siqin, Cheung, Peter Pak-Hang, Bierer, Donald, Zhang, Mingjie, Huang, Xuhui, Li, Xuechen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: RSC 2021
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8341669/
https://www.ncbi.nlm.nih.gov/pubmed/34458841
http://dx.doi.org/10.1039/d1cb00087j
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author Unarta, Ilona Christy
Xu, Jianchao
Shang, Yuan
Cheung, Carina Hey Pui
Zhu, Ruichi
Chen, Xudong
Cao, Siqin
Cheung, Peter Pak-Hang
Bierer, Donald
Zhang, Mingjie
Huang, Xuhui
Li, Xuechen
author_facet Unarta, Ilona Christy
Xu, Jianchao
Shang, Yuan
Cheung, Carina Hey Pui
Zhu, Ruichi
Chen, Xudong
Cao, Siqin
Cheung, Peter Pak-Hang
Bierer, Donald
Zhang, Mingjie
Huang, Xuhui
Li, Xuechen
author_sort Unarta, Ilona Christy
collection PubMed
description Stapled peptides are promising protein–protein interaction (PPI) inhibitors that can increase the binding potency. Different from small-molecule inhibitors in which the binding mainly depends on energetic interactions with their protein targets, the binding of stapled peptides has long been suggested to be benefited from entropy. However, it remains challenging to reveal the molecular features that lead to this entropy gain, which could originate from the stabilization of the stapled peptide in solution or from the increased flexibility of the complex upon binding. This hinders the rational design of stapled peptides as PPI inhibitors. Using the guanylate kinase (GK) domain of the postsynaptic density protein 95 (PSD-95) as the target, we quantified the enthalpic and entropic contributions by combining isothermal titration calorimetry (ITC), X-ray crystallography, and free energy calculations based on all-atom molecular dynamics (MD) simulations. We successfully designed a stapled peptide inhibitor (staple 1) of the PSD-95 GK domain that led to a 25-fold increase in the binding affinity (from tens of μMs to 1.36 μM) with high cell permeability. We showed that entropy indeed greatly enhanced the binding affinity and the entropy gain was mainly due to the constrained-helix structure of the stapled peptide in solution (free state). Based on staple 1, we further designed two other stapled peptides (staple 2 and 3), which exerted even larger entropy gains compared to staple 1 because of their more flexible bound complexes (bound state). However, for staple 2 and 3, the overall binding affinities were not improved, as the loose binding in their bound states led to an enthalpic loss that largely compensated the excess entropy gain. Our work suggests that increasing the stability of the stapled peptide in free solution is an effective strategy for the rational design of stapled peptides as PPI inhibitors.
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spelling pubmed-83416692021-08-26 Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain Unarta, Ilona Christy Xu, Jianchao Shang, Yuan Cheung, Carina Hey Pui Zhu, Ruichi Chen, Xudong Cao, Siqin Cheung, Peter Pak-Hang Bierer, Donald Zhang, Mingjie Huang, Xuhui Li, Xuechen RSC Chem Biol Chemistry Stapled peptides are promising protein–protein interaction (PPI) inhibitors that can increase the binding potency. Different from small-molecule inhibitors in which the binding mainly depends on energetic interactions with their protein targets, the binding of stapled peptides has long been suggested to be benefited from entropy. However, it remains challenging to reveal the molecular features that lead to this entropy gain, which could originate from the stabilization of the stapled peptide in solution or from the increased flexibility of the complex upon binding. This hinders the rational design of stapled peptides as PPI inhibitors. Using the guanylate kinase (GK) domain of the postsynaptic density protein 95 (PSD-95) as the target, we quantified the enthalpic and entropic contributions by combining isothermal titration calorimetry (ITC), X-ray crystallography, and free energy calculations based on all-atom molecular dynamics (MD) simulations. We successfully designed a stapled peptide inhibitor (staple 1) of the PSD-95 GK domain that led to a 25-fold increase in the binding affinity (from tens of μMs to 1.36 μM) with high cell permeability. We showed that entropy indeed greatly enhanced the binding affinity and the entropy gain was mainly due to the constrained-helix structure of the stapled peptide in solution (free state). Based on staple 1, we further designed two other stapled peptides (staple 2 and 3), which exerted even larger entropy gains compared to staple 1 because of their more flexible bound complexes (bound state). However, for staple 2 and 3, the overall binding affinities were not improved, as the loose binding in their bound states led to an enthalpic loss that largely compensated the excess entropy gain. Our work suggests that increasing the stability of the stapled peptide in free solution is an effective strategy for the rational design of stapled peptides as PPI inhibitors. RSC 2021-06-25 /pmc/articles/PMC8341669/ /pubmed/34458841 http://dx.doi.org/10.1039/d1cb00087j Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Unarta, Ilona Christy
Xu, Jianchao
Shang, Yuan
Cheung, Carina Hey Pui
Zhu, Ruichi
Chen, Xudong
Cao, Siqin
Cheung, Peter Pak-Hang
Bierer, Donald
Zhang, Mingjie
Huang, Xuhui
Li, Xuechen
Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title_full Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title_fullStr Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title_full_unstemmed Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title_short Entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the GK domain
title_sort entropy of stapled peptide inhibitors in free state is the major contributor to the improvement of binding affinity with the gk domain
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8341669/
https://www.ncbi.nlm.nih.gov/pubmed/34458841
http://dx.doi.org/10.1039/d1cb00087j
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