The angiotensin II
type 2 receptor (AT
2
R) has attracted
much attention as a potential target for the relief of neuropathic
pain, which represents an area of unmet clinical need. A series of
1,2,3,4-tetrahydroisoquinolines with a benzoxazole side-chain were
discovered as potent AT
2
R antagonists. Rational optimization
resulted in compound
15
, which demonstrated both excellent
antagonistic activity against AT
2
R
in vitro
and analgesic efficacy in a rat chronic constriction injury model.
Its favorable physicochemical properties and oral bioavailability
make it a promising therapeutic candidate for neuropathic pain.
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