What does this research mean for the field?

Steroids can act as generalizable ligands for adhesion GPCRs, suggesting a shared recognition mechanism across this receptor class. Novelty: ClaimNovelty.SYNTHESIS. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

This research examines how steroids interact with adhesion GPCRs and the significance of these interactions.

February 19, 2026Open Access

Steroid Recognition in Adhesion GPCRs : A Structural and Pharmacological Perspective

Key Points

This research examines how steroids interact with adhesion GPCRs and the significance of these interactions.
Reviewed structural evidence from cryo-EM of ADGRD1 bound to steroids.
Conducted comparative docking and homology modeling to assess binding mechanisms.
Analyzed the reproducibility and physiological relevance of steroid binding.
Identified a steroid-binding pocket in ADGRD1.
Developed a selective synthetic agonist based on structural insights.
Highlighted the potential for broader ligand recognition across adhesion GPCRs.

Abstract

ABSTRACT Emerging evidence suggests steroids may act as generalizable ligands for adhesion GPCRs, a receptor class with considerable pharmacological potential. While most studies have focused on the ADGR‘G' subfamily, recent cryo‐EM structures of the androgens 5α‐dihydrotestosterone (5α‐DHT) and methenolone bound to ADGRD1 revealed a putative steroid‐binding pocket and enabled the rational design of a selective synthetic agonist. This perspective considers the broader significance of these findings amid some debate about the reproducibility and physiological relevance of steroid binding to adhesion GPCRs, reviewing all structural evidence and presenting comparative docking and homology modeling to evaluate conserved features and the plausibility of a shared recognition mechanism.

Steroid Recognition in Adhesion GPCRs : A Structural and Pharmacological Perspective

Key Points

Abstract

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