Design, Synthesis,
and Structure–Activity Relationship
Studies of Novel GPR88 Agonists (4-Substituted-phenyl)acetamides Based
on the Reversed Amide Scaffold
The development of synthetic agonists
for the orphan
receptor GPR88
has recently attracted significant interest, given the promise of
GPR88 as a novel drug target for psychiatric and neurodegenerative
disorders. Examination of structure–activity relationships
of two known agonist scaffolds 2-PCCA and 2-AMPP, as well as the recently
resolved cryo-EM structure of 2-PCCA-bound GPR88, led to the design
of a new scaffold based on the “reversed amide” strategy
of 2-AMPP. A series of novel (4-substituted-phenyl)acetamides were
synthesized and assessed in cAMP accumulation assays as GPR88 agonists,
which led to the discovery of several compounds with better or comparable
potencies to 2-AMPP. Computational docking studies suggest that these
novel GPR88 agonists bind to the same allosteric site of GPR88 that
2-PCCA occupies. Collectively, our findings provide structural insight
and SAR requirement at the allosteric site of GPR88 and a new scaffold
for further development of GPR88 allosteric agonists