Functional coupling of the nociceptin/orphanin FQ receptor in dog brain membranes

Nociceptin/orphanin FQ (N/OFQ) is the endogenous ligand for the N/OFQ receptor (NOP) which is yet to be functionally characterized in dog brain. Ligand binding data reports low NOP density (29 fmol mg 1 protein) in dog. In this study using dog brain membranes, we have examined the effects of N/OFQ on [leucyl-3H]N/OFQ(1–17)OH ([leucyl-3H]N/OFQ) binding in the presence and absence of 120 mM NaCl and 100 AM GTPgS. Data from standard [35S]GTPgS binding and immunoprecipitation (Gai1 – 3) assays are also presented, along with data from a limited number of control experiments with human NOP expressed in Chinese hamster ovary (CHOhNOP) cells. N/OFQ displaced [leucyl-3H]N/OFQ binding with pKi and slope values of 9.62F0.07 and 0.38F0.05, respectively. Addition of NaCl/GTPgS produced a steepening (slope 0.95F0.06, n = 3) of the curve. N/OFQ stimulated [35S]GTPgS binding with pEC50 and Emax values of 8.21F0.17 and 1.17F0.01, respectively (in CHOhNOP, pEC50 and Emax values were 8.47F0.01 and 7.01F0.63). N/OFQ stimulated [35S]GTPgS binding in dog and CHOhNOP cell membranes could be immunoprecipitated with an anti-Gai1 – 3 antibody, indicating coupling to a pertussis toxin (PTx)-sensitive G-protein. N/OFQ actions were competitively antagonized by the selective NOP antagonists, 100 nM J-113397, 1 AM [Nphe1]N/OFQ(1–13)NH2 and 1 AM [Phe1C(CH2-NH)Gly2]N/OFQ(1–13)NH2 (partial agonist) yielding pKB values of 8.58F0.21, 7.06F0.59 and 7.32F0.41, respectively (in CHOhNOP, a pKB for J-113397 of 8.33F0.02 was obtained). Despite relatively low receptor density, we were able to detect functional activity of native dog NOP, with pharmacology consistent with reports for other species.