Discovery of δ Opioid Receptor Full Inverse Agonists and Their Effects on Restraint Stress-Induced Cognitive Impairment in Mice.

Shigeto HirayamaTakashi IwaiEika HigashiMinami NakamuraChiharu IwamatsuKennosuke ItohToru NemotoMitsuo TanabeHideaki Fujii

Published in: ACS chemical neuroscience (2019)

The cyclopropylmethyl group in classical δ opioid receptor (DOR) antagonist NTI, BNTX, and NTB was replaced with various electron-withdrawing groups to develop DOR inverse agonists. N-Benzyl NTB derivative SYK-657 was a potent DOR full inverse agonist and its potency was over 10-fold potent than that of a reference compound ICI-174,864. Intraperitoneal administration of SYK-657 induced the short-term memory improving effect in mice without abnormal behaviors.

Keyphrases

stress induced
cognitive impairment
chronic pain
pain management
high fat diet induced
tyrosine kinase
small molecule
anti inflammatory
high glucose
diabetic rats
binding protein
type diabetes
endothelial cells
oxidative stress
skeletal muscle
electron microscopy