Discovery of a cryptic pocket in the AI-predicted structure of PPM1D phosphatase explains the binding site and potency of its allosteric inhibitors

Artur Meller; Saulo De Oliveira; Aram Davtyan; Tigran Abramyan; Gregory R Bowman; Henry van den Bedem

doi:10.3389/fmolb.2023.1171143

Discovery of a cryptic pocket in the AI-predicted structure of PPM1D phosphatase explains the binding site and potency of its allosteric inhibitors

Front Mol Biosci. 2023 Apr 18:10:1171143. doi: 10.3389/fmolb.2023.1171143. eCollection 2023.

Authors

Artur Meller^{1

2}, Saulo De Oliveira³, Aram Davtyan³, Tigran Abramyan³, Gregory R Bowman⁴, Henry van den Bedem^{3

5}

Affiliations

¹ Department of Biochemistry and Molecular Biophysics, Washington University in St. Louis, St. Louis, MO, United States.
² Medical Scientist Training Program, Washington University in St. Louis, St. Louis, MO, United States.
³ Atomwise, Inc., San Francisco, CA, United States.
⁴ Department of Biochemistry and Biophysics, University of Pennsylvania, Philadelphia, PA, United States.
⁵ Department of Bioengineering and Therapeutic Sciences, University of California, San Francisco, CA, United States.

Abstract

Virtual screening is a widely used tool for drug discovery, but its predictive power can vary dramatically depending on how much structural data is available. In the best case, crystal structures of a ligand-bound protein can help find more potent ligands. However, virtual screens tend to be less predictive when only ligand-free crystal structures are available, and even less predictive if a homology model or other predicted structure must be used. Here, we explore the possibility that this situation can be improved by better accounting for protein dynamics, as simulations started from a single structure have a reasonable chance of sampling nearby structures that are more compatible with ligand binding. As a specific example, we consider the cancer drug target PPM1D/Wip1 phosphatase, a protein that lacks crystal structures. High-throughput screens have led to the discovery of several allosteric inhibitors of PPM1D, but their binding mode remains unknown. To enable further drug discovery efforts, we assessed the predictive power of an AlphaFold-predicted structure of PPM1D and a Markov state model (MSM) built from molecular dynamics simulations initiated from that structure. Our simulations reveal a cryptic pocket at the interface between two important structural elements, the flap and hinge regions. Using deep learning to predict the pose quality of each docked compound for the active site and cryptic pocket suggests that the inhibitors strongly prefer binding to the cryptic pocket, consistent with their allosteric effect. The predicted affinities for the dynamically uncovered cryptic pocket also recapitulate the relative potencies of the compounds (τ_b = 0.70) better than the predicted affinities for the static AlphaFold-predicted structure (τ_b = 0.42). Taken together, these results suggest that targeting the cryptic pocket is a good strategy for drugging PPM1D and, more generally, that conformations selected from simulation can improve virtual screening when limited structural data is available.

Keywords: allosteric inhibition; cryptic site; deep learning; markov state models; molecular dynamics simulation; virtual high throughput screening (vHTS).

Grants and funding

F30 HL162431/HL/NHLBI NIH HHS/United States