Molecular determinants of antagonist interactions with chemokine receptors CCR2 and CCR5

John R D Dawson; Grant M Wadman; Penglie Zhang; Andrew Tebben; Percy H Carter; Siyi Gu; Thomas Shroka; Leire Borrega-Roman; Catherina L Salanga; Tracy M Handel; Irina Kufareva

doi:10.1101/2023.11.15.567150

Molecular determinants of antagonist interactions with chemokine receptors CCR2 and CCR5

bioRxiv [Preprint]. 2024 Feb 12:2023.11.15.567150. doi: 10.1101/2023.11.15.567150.

Authors

John R D Dawson¹, Grant M Wadman¹, Penglie Zhang², Andrew Tebben³, Percy H Carter^{3

4}, Siyi Gu^{1

5}, Thomas Shroka^{1

6}, Leire Borrega-Roman¹, Catherina L Salanga¹, Tracy M Handel¹, Irina Kufareva¹

Affiliations

¹ Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California San Diego, La Jolla, CA, USA.
² ChemoCentryx, Mountain View, CA, USA.
³ Bristol Myers Squibb Company, Princeton, NJ, USA.
⁴ (current affiliation) Blueprint Medicines, Cambridge, MA, USA.
⁵ (current affiliation) Lycia Therapeutics, South San Francisco, CA.
⁶ (current affiliation) Avidity Biosciences Inc., San Diego, CA.

Abstract

By driving monocyte chemotaxis, the chemokine receptor CCR2 shapes inflammatory responses and the formation of tumor microenvironments. This makes it a promising target in inflammation and immuno-oncology; however, despite extensive efforts, there are no FDA-approved CCR2-targeting therapeutics. Cited challenges include the redundancy of the chemokine system, suboptimal properties of compound candidates, and species differences that confound the translation of results from animals to humans. Structure-based drug design can rationalize and accelerate the discovery and optimization of CCR2 antagonists to address these challenges. The prerequisites for such efforts include an atomic-level understanding of the molecular determinants of action of existing antagonists. In this study, using molecular docking and artificial-intelligence-powered compound library screening, we uncover the structural principles of small molecule antagonism and selectivity towards CCR2 and its sister receptor CCR5. CCR2 orthosteric inhibitors are shown to universally occupy an inactive-state-specific tunnel between receptor helices 1 and 7; we also discover an unexpected role for an extra-helical groove accessible through this tunnel, suggesting its potential as a new targetable interface for CCR2 and CCR5 modulation. By contrast, only shape complementarity and limited helix 8 hydrogen bonding govern the binding of various chemotypes of allosteric antagonists. CCR2 residues S101^2.63 and V244^6.36 are implicated as determinants of CCR2/CCR5 and human/mouse orthosteric and allosteric antagonist selectivity, respectively, and the role of S101^2.63 is corroborated through experimental gain-of-function mutagenesis. We establish a critical role of induced fit in antagonist recognition, reveal strong chemotype selectivity of existing structures, and demonstrate the high predictive potential of a new deep-learning-based compound scoring function. Finally, this study expands the available CCR2 structural landscape with computationally generated chemotype-specific models well-suited for structure-based antagonist design.

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Preprint

Abstract

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