Inhibition of TRPM8 function by prostacyclin receptor agonists requires 
coupling to Gq/11 proteins

Trif, Cosmin; Banica, Alexandra-Maria; Manolache, Alexandra; Anghel, Sorina Andreea; Hutanu, Debora-Elena; Stratulat, Teodora; Badea, Rodica; Oprita, George; Selescu, Tudor; Petrescu, Stefana M.; Sisignano, Marco; Offermanns, Stefan; Babes, Alexandru; Tunaru , Sorin

doi:10.1111/bph.16295

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Inhibition of TRPM8 function by prostacyclin receptor agonists requires coupling to Gq/11 proteins

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Offermanns, Stefan
Pharmacology, Max Planck Institute for Heart and Lung Research, Max Planck Society;

Tunaru , Sorin
Pharmacology, Max Planck Institute for Heart and Lung Research, Max Planck Society;

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Zitation

Trif, C., Banica, A.-M., Manolache, A., Anghel, S. A., Hutanu, D.-E., Stratulat, T., et al. (2023). Inhibition of TRPM8 function by prostacyclin receptor agonists requires coupling to Gq/11 proteins. BRITISH JOURNAL OF PHARMACOLOGY. doi:10.1111/bph.16295.

Zitierlink: https://hdl.handle.net/21.11116/0000-000E-61E1-6

Zusammenfassung

Background and PurposeThe TRPM8 ion channel is involved in innocuous cold sensing and has a potent anti-inflammatory action. Its activation by lower temperature or chemical agonists such as menthol and icilin induces analgesic effects, reversing hypersensitivity and reducing chronic pain. On the other hand, prostacyclin (PGI2) enhances pain and inflammation by activating the IP receptors. Due to the critical roles of TRPM8 and IP receptors in the regulation of inflammatory pain, and considering their overlapping expression pattern, we analysed the functional interaction between human TRPM8 and IP receptors.Experimental ApproachWe transiently expressed human TRPM8 channels and IP receptors in HEK293T cells and carried out intracellular calcium and cAMP measurements. Additionally, we cultured neurons from the dorsal root ganglia (DRGs) of mice and determined the increase in intracellular calcium triggered by the TRPM8 agonist, icilin, in the presence of the IP receptor agonist cicaprost, the IP receptor antagonist Cay10441, and the Gq/11 inhibitor YM254890.Key ResultsActivation of IP receptors by selective agonists (cicaprost, beraprost, and iloprost) inhibited TRPM8 channel function, independently of the Gs-cAMP pathway. The potent inhibition of TRPM8 channels by IP receptor agonists involved Gq/11 coupling. These effects were also observed in neurons isolated from murine DRGs.Conclusions and ImplicationsOur results demonstrate an unusual signalling pathway of IP receptors by coupling to Gq/11 proteins to inhibit TRPM8 channel function. This pathway may contribute to a better understanding of the role of TRPM8 channels and IP receptors in regulating pain and inflammation.