Small molecule ligands targetting GPR171 alone do not produce antinociception. GPR171 agonist (MS15203; 10 mg/kg, i.p.), GPR171 antagonist (MS21570; 5 mg/kg, i.p), or vehicle (10% DMSO in saline, i.p.) were administered to mice and then tested on the warm water (52°C) tail flick assay (A) or hot plate (50°C) assay (B) at 15, 30, 60, or 120 minute. The data reveal no change in nociception on either test. Data are the means ± S.E. of 8–12 animals/group.

GPR171 ligands alter morphine antinociception. GPR171 agonist (MS15203; 10 mg/kg, i.p.), GPR171 antagonist (MS21570; 5 mg/kg, i.p), or vehicle (10% DMSO in saline, i.p.) were administered 10 minutes prior to saline (10 ml/kg) or morphine (Mor; 2 or 5 mg/kg, s.c.). Antinociception was evaluated at 15, 30, 60, or 120 minutes on the warm water (52°C) tail flick assay (A) or hot plate (50°C) assay (B). GPR171 agonist, MS15203, does not alter morphine (5 mg)-induced antinociception while GPR171 antagonist decreases antinociception as measured on the tail flick assay. MS15203 increases antinociception following the lower dose of morphine (2 mg). (B) On the hot plate test, MS15203 increases 5 mg morphine-induced antinociception at 15, 30, and 60 minutes, while MS21570+Mor (5 mg) does not induce antinociception greater than saline controls. MS15203+Mor (2 mg) produced significant antinociception at 30 minutes, whereas Mor (2 mg) did not. Inset: Dunnett’s post hoc to evaluate main effect compared with saline. *P< 0.05; ***P < 0.001; ****P < 0.0001, compared with saline; #P<0.05, compared with morphine; @P<0.05, compared with morphine + agonist. n.s., Not significant; HP, hot plate; TF, tail flick. Data are the means ± S.E. of 8–15 animals/group.

GPR171 ligands do not bind or signal at the MOPr . Displacement binding assays were carried out with membranes (50 μg protein) from CHO cells stably expressing either MOPr (A) or GPR171 (B) using [³H]DAMGO (3 nM final concentration) in the absence or presence of either 10 μM DAMGO, MS15203, or MS21570 as described in Materials and Methods. Data shows that MS15203 and MS21570 do not bind to MOPr and DAMGO does not bind to GPR171. (C) Membranes (20 μg protein) from CHO cells stably expressing MOPr were subjected to a [³⁵S]GTPγS binding assay using DAMGO (0–10 μM) in the absence or presence of 10 μM MS21570 as described in Materials and Methods. Data shows that MS21570 does not affect signaling by DAMGO in cells only expressing MOPr. E_max was calculated at 10 μM DAMGO. Data are mean ± S.E. of three experiments in triplicate. ****P < 0.0001; one-way ANOVA; n.s., not significant.