Identification of a preassembled TRH receptor-G q/11 protein complex in HEK293 cells

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Abstract

Protein-protein interactions define specificity in signal transduction and these interactions are central to transmembrane signaling by G-protein-coupled receptors (GPCRs). It is not quite clear, however, whether GPCRs and the regulatory trimeric G-proteins behave as freely and independently diffusible molecules in the plasma membrane or whether they form some preassociated complexes. Here we used clear-native polyacrylamide gel electrophoresis (CN-PAGE) to investigate the presumed coupling between thyrotropin-releasing hormone (TRH) receptor and its cognate G q/11 protein in HEK293 cells expressing high levels of these proteins. Under different solubilization conditions, the TRH receptor (TRH-R) was identified to form a putative pentameric complex composed of TRH-R homodimer and G q/11 protein. The presumed association of TRH-R with G q/11α or Gβ proteins in plasma membranes was verified by RNAi experiments. After 10- or 30-min hormone treatment, TRH-R signaling complexes gradually dissociated with a concomitant release of receptor homodimers. These observations support the model in which GPCRs can be coupled to trimeric G-proteins in preassembled signaling complexes, which might be dynamically regulated upon receptor activation. The precoupling of receptors with their cognate G-proteins can contribute to faster G-protein activation and infsequent signal transfer into the cell interior. © 2012 by Japan Society for Cell Biology.

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Drastichova, Z., & Novotny, J. (2012). Identification of a preassembled TRH receptor-G q/11 protein complex in HEK293 cells. Cell Structure and Function, 37(1), 1–12. https://doi.org/10.1247/csf.11024

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