Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.

Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.

In this study we wanted to gain insights into selectivity mechanisms between G-protein-coupled receptors (GPCR) and different subtypes of G-proteins. The thyrotropin receptor (TSHR) binds G-proteins promiscuously and activates both Gs (cAMP) and Gq (IP). Our goal was to dissect selectivity patterns...

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Main Authors: Gunnar Kleinau, Holger Jaeschke, Catherine L Worth, Sandra Mueller, Jorge Gonzalez, Ralf Paschke, Gerd Krause
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2841179?pdf=render
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spelling doaj-6375b17bcdb04d76b69203b1abe1ceac2020-11-24T21:46:42ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-01-0153e974510.1371/journal.pone.0009745Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.Gunnar KleinauHolger JaeschkeCatherine L WorthSandra MuellerJorge GonzalezRalf PaschkeGerd KrauseIn this study we wanted to gain insights into selectivity mechanisms between G-protein-coupled receptors (GPCR) and different subtypes of G-proteins. The thyrotropin receptor (TSHR) binds G-proteins promiscuously and activates both Gs (cAMP) and Gq (IP). Our goal was to dissect selectivity patterns for both pathways in the intracellular region of this receptor. We were particularly interested in the participation of poorly investigated receptor parts.We systematically investigated the amino acids of intracellular loop (ICL) 1 and helix 8 using site-directed mutagenesis alongside characterization of cAMP and IP accumulation. This approach was guided by a homology model of activated TSHR in complex with heterotrimeric Gq, using the X-ray structure of opsin with a bound G-protein peptide as a structural template.We provide evidence that ICL1 is significantly involved in G-protein activation and our model suggests potential interactions with subunits G alpha as well as G betagamma. Several amino acid substitutions impaired both IP and cAMP accumulation. Moreover, we found a few residues in ICL1 (L440, T441, H443) and helix 8 (R687) that are sensitive for Gq but not for Gs activation. Conversely, not even one residue was found that selectively affects cAMP accumulation only. Together with our previous mutagenesis data on ICL2 and ICL3 we provide here the first systematically completed map of potential interfaces between TSHR and heterotrimeric G-protein. The TSHR/Gq-heterotrimer complex is characterized by more selective interactions than the TSHR/Gs complex. In fact the receptor interface for binding Gs is a subset of that for Gq and we postulate that this may be true for other GPCRs coupling these G-proteins. Our findings support that G-protein coupling and preference is dominated by specific structural features at the intracellular region of the activated GPCR but is completed by additional complementary recognition patterns between receptor and G-protein subtypes.http://europepmc.org/articles/PMC2841179?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Gunnar Kleinau
Holger Jaeschke
Catherine L Worth
Sandra Mueller
Jorge Gonzalez
Ralf Paschke
Gerd Krause
spellingShingle Gunnar Kleinau
Holger Jaeschke
Catherine L Worth
Sandra Mueller
Jorge Gonzalez
Ralf Paschke
Gerd Krause
Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
PLoS ONE
author_facet Gunnar Kleinau
Holger Jaeschke
Catherine L Worth
Sandra Mueller
Jorge Gonzalez
Ralf Paschke
Gerd Krause
author_sort Gunnar Kleinau
title Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
title_short Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
title_full Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
title_fullStr Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
title_full_unstemmed Principles and determinants of G-protein coupling by the rhodopsin-like thyrotropin receptor.
title_sort principles and determinants of g-protein coupling by the rhodopsin-like thyrotropin receptor.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-01-01
description In this study we wanted to gain insights into selectivity mechanisms between G-protein-coupled receptors (GPCR) and different subtypes of G-proteins. The thyrotropin receptor (TSHR) binds G-proteins promiscuously and activates both Gs (cAMP) and Gq (IP). Our goal was to dissect selectivity patterns for both pathways in the intracellular region of this receptor. We were particularly interested in the participation of poorly investigated receptor parts.We systematically investigated the amino acids of intracellular loop (ICL) 1 and helix 8 using site-directed mutagenesis alongside characterization of cAMP and IP accumulation. This approach was guided by a homology model of activated TSHR in complex with heterotrimeric Gq, using the X-ray structure of opsin with a bound G-protein peptide as a structural template.We provide evidence that ICL1 is significantly involved in G-protein activation and our model suggests potential interactions with subunits G alpha as well as G betagamma. Several amino acid substitutions impaired both IP and cAMP accumulation. Moreover, we found a few residues in ICL1 (L440, T441, H443) and helix 8 (R687) that are sensitive for Gq but not for Gs activation. Conversely, not even one residue was found that selectively affects cAMP accumulation only. Together with our previous mutagenesis data on ICL2 and ICL3 we provide here the first systematically completed map of potential interfaces between TSHR and heterotrimeric G-protein. The TSHR/Gq-heterotrimer complex is characterized by more selective interactions than the TSHR/Gs complex. In fact the receptor interface for binding Gs is a subset of that for Gq and we postulate that this may be true for other GPCRs coupling these G-proteins. Our findings support that G-protein coupling and preference is dominated by specific structural features at the intracellular region of the activated GPCR but is completed by additional complementary recognition patterns between receptor and G-protein subtypes.
url http://europepmc.org/articles/PMC2841179?pdf=render
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