Issue 6, 2024

Ancient and modern mechanisms compete in progesterone receptor activation

Abstract

The progesterone receptor (PR) belongs to the steroid receptor family of ligand-regulated transcription factors, controlling genes important for development, metabolism, and reproduction. Understanding how diverse ligands bind and modulate PR activity will illuminate the design of ligands that control PR-driven signaling pathways. Here, we use molecular dynamics simulations to investigate how PR dynamics are altered by functionally diverse ligands. Using a library of 33 steroidal ligands that range from inactive to EC50 < 0.1 nM, we reveal an unexpected evolutionary basis for the wide gamut of activation. While other oxosteroid receptors employ an evolutionarily conserved mechanism dependent on a hydrogen bond between the receptor and ligand, extant PR has evolved a preference for activation that is not reliant on this polar interaction. We demonstrate that potent ligands utilize the modern PR mechanism while weaker ligands coopt the defunct ancestral mechanism by forming hydrogen bonds with Asn719. Based on their structures and dynamic signatures, ligands partition into four classes (inactive, weak, moderate and high potency) that interact distinctly with the PR binding pocket. Further, we use luciferase reporter assays and PR mutants to probe the roles of pocket residues in mediating distinct PR mechanisms. This combination of MD simulations and in vitro studies provide insight into how the evolutionary history of PR shapes its response to diverse ligands.

Graphical abstract: Ancient and modern mechanisms compete in progesterone receptor activation

Supplementary files

Article information

Article type
Paper
Submitted
28 fev 2024
Accepted
27 mar 2024
First published
15 apr 2024
This article is Open Access
Creative Commons BY-NC license

RSC Chem. Biol., 2024,5, 518-529

Ancient and modern mechanisms compete in progesterone receptor activation

S. H. Khan, N. Dube, N. Sudhakar, O. Fraser, P. Villalona, S. M. Braet, S. Leedom, E. R. Reilly, J. Sivak, K. Crittenden and C. D. Okafor, RSC Chem. Biol., 2024, 5, 518 DOI: 10.1039/D4CB00002A

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