Transient receptor potential M3 channels are ionotropic steroid receptors in pancreatic beta cells

瞬时受体电位 M3 通道是胰腺 β 细胞中的离子型类固醇受体

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作者:Thomas F J Wagner, Sabine Loch, Sachar Lambert, Isabelle Straub, Stefanie Mannebach, Ilka Mathar, Martina Düfer, Annette Lis, Veit Flockerzi, Stephan E Philipp, Johannes Oberwinkler

Abstract

Transient receptor potential (TRP) cation channels are renowned for their ability to sense diverse chemical stimuli. Still, for many members of this large and heterogeneous protein family it is unclear how their activity is regulated and whether they are influenced by endogenous substances. On the other hand, steroidal compounds are increasingly recognized to have rapid effects on membrane surface receptors that often have not been identified at the molecular level. We show here that TRPM3, a divalent-permeable cation channel, is rapidly and reversibly activated by extracellular pregnenolone sulphate, a neuroactive steroid. We show that pregnenolone sulphate activates endogenous TRPM3 channels in insulin-producing beta cells. Application of pregnenolone sulphate led to a rapid calcium influx and enhanced insulin secretion from pancreatic islets. Our results establish that TRPM3 is an essential component of an ionotropic steroid receptor enabling unanticipated crosstalk between steroidal and insulin-signalling endocrine systems.

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