Activation of dimerized BRS3-EP3 suppresses melanoma cell migration through coupling Gα(s) protein.

The mechanism underlying the crosstalk between Gα(q)-coupled bombesin receptor subtype-3 (BRS3) and Gα(i)-coupled E-prostanoid 3 receptor (EP3) remains unknown. Here, we report that BRS3 and EP3 form dimers in the membrane of living HEK-293T cells. BRS3-EP3 dimers switched to couple Gα(s) protein upon PGE2 stimulation, which provoked cAMP accumulation and enhanced P38 phosphorylation. Quantitative proteomics analysis revealed that the activation of BRS3-EP3 dimers was associated with cell migration. B16 melanoma cell line, which endogenously expresses BRS3 and EP3, was selected to investigate the function of BRS3-EP3 dimers. The results demonstrated that the presence of BRS3 inhibited the migration of B16 melanoma cells upon PGE2 stimulation. Utilizing inhibitors of Gα(s) and P38, we found that BRS3 interacted with EP3 and switched to couple Gα(s) protein, causing P38 phosphorylation to inhibit F-actin rearrangement and ultimately suppressed cell migration. Our study reveals the crosstalk between the orphan receptor BRS3 and EP3, and provides a potential novel target for disease treatment.