1 research outputs found
Ligand-Based Discovery of a New Scaffold for Allosteric Modulation of the μ‑Opioid Receptor
With
the hope of discovering effective analgesics with fewer side
effects, attention has recently shifted to allosteric modulators of
the opioid receptors. In the past two years, the first chemotypes
of positive or silent allosteric modulators (PAMs or SAMs, respectively)
of μ- and δ-opioid receptor types have been reported in
the literature. During a structure-guided lead optimization campaign
with μ-PAMs BMS-986121 and BMS-986122 as starting compounds,
we discovered a new chemotype that was confirmed to display μ-PAM
or μ-SAM activity depending on the specific substitutions as
assessed by endomorphin-1-stimulated β-arrestin2 recruitment
assays in Chinese Hamster Ovary (CHO)-μ PathHunter cells. The
most active μ-PAM of this series was analyzed further in competition
binding and G-protein activation assays to understand its effects
on ligand binding and to investigate the nature of its probe dependence