TRP Genes

Author:

Qian Feng1,Huang Ping1,Ma Li2,Kuznetsov Andrey2,Tamarina Natalia2,Philipson Louis H.2

Affiliation:

1. Department of Neurobiology, Physiology, and Pharmacology, the University of Chicago, Chicago, Illinois

2. Department of Medicine and Committee in Cell Physiology, the University of Chicago, Chicago, Illinois

Abstract

Nonselective cation channels may play a role in insulin secretion by regulating pancreatic β-cell plasma membrane potential, Ca2+ homeostasis, and thereby glucose signaling. Transient receptor potential channel (TRPC)-related genes encode nonselective cation channels, some of which are similar to those described for β-cells. Some TRPC-like channels are activated via G-protein–coupled mechanisms, some have been reported to be calcium-store–operated channels (SOC), and others are activated by novel signaling molecules or are sensitive to pressure and osmotic strength. Here we report the cloning and expression of mSTRPC4 from a mouse insulinoma cDNA library. mSTRPC4 encoded a protein of 97 kd, expressed in both endocrine cells and the brain. Stable cell lines expressing mSTRPC4 showed abundant mSTRPC4 protein, but no reproducible currents could be detected. mSTRPC4 therefore probably functions as a heteromultimer. We also report that LTRPC2, a G-protein and adenosine 5′-diphosphoribose (ADPR)-activated nonselective cation channel, is also expressed in human islets. TRPC-like channels may provide a pathway for depolarization or Ca2+ entry in β-cells and may be interesting targets for manipulating β-cell function.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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