The G-protein GPCR signaling is important in nociceptive modulation as well as in pain generation. A variety of key nociceptive modulators are known to activate GPCRs expressed on sensory nerves. Because these neuromodulators can activate the Gq/11, Gs, Gi/o as well as the G12/13 branches of G-protein signaling, the relative contribution and functional significance of the individual signaling pathways in modulation of nociceptor function in vivo is not clear. Using nociceptor-specific Gáq/11-deficient mice, we found recently that Gáq/11 signaling tonically modulates baseline nociceptor function, contributes to acute and chronic inflammatory sensitization and modulates voltage gated-sodium channels. In this project we plan to identify the mechanisms of Gáq/11-mediated modulation of voltage gated-sodium channels. Furthermore, we plan to perform profiling experiments to elucidate the role of Gáq/11 in gene regulation. Using patch-clamp electrophysiological recordings, we aim at investigating the influence of Gáq/11 signaling on nociceptor properties. We will unravel the individual role of Gáq and Gá11 in signal transduction in nociceptors and finally investigate the role of Gáq/11 in clinically relevant models of chronic pain. This project will deliver detailed insights into the functional contribution of Gáq/11 signaling in nociceptors towards the development of peripheral sensitization as well as the induction of central sensitization, which represents critically important aspects of the pathophysiology of chronic pain.

DFG Programme Research Grants