The TRPM7 channel is inactivated by PIP2 hydrolysis

Author:  ["Loren W. Runnels","Lixia Yue","David E. Clapham"]

Publication:  Nature Cell Biology

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Abstract

TRPM7 (ChaK1, TRP-PLIK, LTRPC7) is a ubiquitous, calcium-permeant ion channel that is unique in being both an ion channel and a serine/threonine kinase. The kinase domain of TRPM7 directly associates with the C2 domain of phospholipase C (PLC). Here, we show that in native cardiac cells and heterologous expression systems, Gαq-linked receptors or tyrosine kinase receptors that activate PLC potently inhibit channel activity. Numerous experimental approaches demonstrated that phosphatidylinositol 4,5-bisphosphate (PIP2), the substrate of PLC, is a key regulator of TRPM7. We conclude that receptor-mediated activation of PLC results in the hydrolysis of localized PIP2, leading to inactivation of the TRPM7 channel.

Cite this article

Runnels, L., Yue, L. & Clapham, D. The TRPM7 channel is inactivated by PIP2 hydrolysis. Nat Cell Biol 4, 329–336 (2002). https://doi.org/10.1038/ncb781

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