PuSH - Publication Server of Helmholtz Zentrum München

Export: TXT Text RIS Endnote (RIS) BIB BibTeX
Müller, A.* ; Kleinau, G.* ; Piechowski, C.L.* ; Müller, T.D. ; Finan, B. ; Pratzka, J.* ; Grüters, A.* ; Krude, H.* ; Tschöp, M.H. ; Biebermann, H.*

G-Protein coupled Receptor 83 (GPR83) signaling determined by constitutive and zinc(II)-induced activity.

PLoS ONE 8:e53347 (2013)
Publ. Version/Full Text Volltext To article DOI PMC
Open Access Gold
Creative Commons Lizenzvertrag
The G-protein coupled receptor 83 (GPR83) is an orphan G-protein coupled receptor for which the natural ligand(s) and signaling pathway(s) remain to be identified. Previous studies suggest a role of GPR83 in the regulation of thermogenesis and the control of circulating adiponectin. The aim of this study was to gain insights into the molecular underpinnings underlying GPR83 signaling. In particular, we aimed to assess the underlying G-protein activated signaling pathway of GPR83 and how this pathway is affected by mutational activation and zinc(II) challenge. Finally, we assessed the capacity of GPR83 for homodimerization. Our results show for the first time that mouse (m) GPR83 has high basal Gq/11 activity without affecting Gi or Gs signaling. Furthermore, we found that, under physiological conditions, zinc(II) (but not calcium(II) and magnesium(II)) potently activates mGPR83, thus identifying zinc(II) as an endogenous molecule with agonistic capability to activate mGPR83. In line with the observation that zinc(II)-ions activate mGPR83, we identified a cluster of ion-binding sensitive amino acids (e.g. His145, His204, Cys207, Glu217) in an activation sensitive receptor region of mGPR83. The occurrence of a constitutive activating mutant and a zinc(II)-binding residue at the N-terminal part corroborate the importance of this region in mGPR83 signal regulation. Finally, our results indicate that mGPR83 forms homodimers, which extend the current knowledge and molecular facets of GPR83 signaling.
Impact Factor
Scopus SNIP
Web of Science
Times Cited
Scopus
Cited By
Altmetric
3.730
1.148
18
18
Tags
Annotations
Special Publikation
Hide on homepage

Edit extra information
Edit own tags
Private
Edit own annotation
Private
Hide on publication lists
on hompage
Mark as special
publikation
Publication type Article: Journal article
Document type Scientific Article
Keywords Glucocorticoid-induced Receptor ; Toggle Switch Model ; Jp05 Messenger-rna ; Extracellular Loops ; Molecular-mechanism ; Structural Biology ; Crystal-structures ; Homology Model ; Cyclic-amp ; T-cells
Language english
Publication Year 2013
HGF-reported in Year 2013
ISSN (print) / ISBN 1932-6203
Journal PLoS ONE
Quellenangaben Volume: 8, Issue: 1, Pages: , Article Number: e53347 Supplement: ,
Publisher Public Library of Science (PLoS)
Publishing Place Lawrence, Kan.
Reviewing status Peer reviewed
Institute(s) Institute of Diabetes and Obesity (IDO)
POF-Topic(s) 30201 - Metabolic Health
Research field(s) Helmholtz Diabetes Center
PSP Element(s) G-502200-001
PubMed ID 23335960
DOI 10.1371/journal.pone.0053347
WOS ID WOS:000314707700014
Scopus ID 84872425037
Permalink https://www.scienceopen.com/document?vid=7b1b6720-dd37-456a-82da-3e3572fb16e7
Erfassungsdatum 2013-03-15
[➜Report correction]