Biased signaling through G-protein-coupled PROKR2 receptors harboring missense mutations.

[kallmann syndrome]

Various missense mutations in the gene coding for prokineticin receptor 2 (PROKR 2 ), a G-protein-coupled receptor , have been identified in patients with Kallmann syndrome . However , the functional consequences of these mutations on the different signaling pathways of this receptor have not been studied . We first showed that the wild-type PROKR 2 can activate different G-protein subtypes (Gq , Gs , and Gi /o ) and recruit β-arrestins in transfected HEK-293 cells . We then examined , for each of these signaling pathways , the effects of 9 mutations that did not significantly impair cell surface targeting or ligand binding of the receptor . Four mutant receptors showing defective Gq signaling (R 85 C , R 85 H , R 164 Q , and V 331 M ) could still recruit β-arrestins on ligand activation , which may cause biased signaling in vivo . Conversely , the R 80 C receptor could activate the 3 types of G proteins but could not recruit β-arrestins . Finally , the R 268 C receptor could recruit β-arrestins and activate the Gq and Gs signaling pathways but could not activate the Gi /o signaling pathway . Our results validate the concept that mutations in the genes encoding membrane receptors can bias downstream signaling in various ways , possibly leading to pathogenic and , perhaps in some cases , protective (e .g ., R 268 C ) effects .