7tm receptors
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Author(s):  
Ségolène Galandrin ◽  
Lauriane Onfroy ◽  
Mathias Charles Poirot ◽  
Jean-Michel Sénard ◽  
Céline Galés
Keyword(s):  

2012 ◽  
Vol 287 (42) ◽  
pp. 35470-35483 ◽  
Author(s):  
Tau Benned-Jensen ◽  
Christoffer Norn ◽  
Stephane Laurent ◽  
Christian M. Madsen ◽  
Hjalte M. Larsen ◽  
...  

Oxysterols are oxygenated cholesterol derivates that are emerging as a physiologically important group of molecules. Although they regulate a range of cellular processes, only few oxysterol-binding effector proteins have been identified, and the knowledge of their binding mode is limited. Recently, the family of G protein-coupled seven transmembrane-spanning receptors (7TM receptors) was added to this group. Specifically, the Epstein-Barr virus-induced gene 2 (EBI2 or GPR183) was shown to be activated by several oxysterols, most potently by 7α,25-dihydroxycholesterol (7α,25-OHC). Nothing is known about the binding mode, however. Using mutational analysis, we identify here four key residues for 7α,25-OHC binding: Arg-87 in TM-II (position II:20/2.60), Tyr-112 and Tyr-116 (positions III:09/3.33 and III:13/3.37) in TM-III, and Tyr-260 in TM-VI (position VI:16/6.51). Substituting these residues with Ala and/or Phe results in a severe decrease in agonist binding and receptor activation. Docking simulations suggest that Tyr-116 interacts with the 3β-OH group in the agonist, Tyr-260 with the 7α-OH group, and Arg-87, either directly or indirectly, with the 25-OH group, although nearby residues likely also contribute. In addition, Tyr-112 is involved in 7α,25-OHC binding but via hydrophobic interactions. Finally, we show that II:20/2.60 constitutes an important residue for ligand binding in receptors carrying a positively charged residue at this position. This group is dominated by lipid- and nucleotide-activated receptors, here exemplified by the CysLTs, P2Y12, and P2Y14. In conclusion, we present the first molecular characterization of oxysterol binding to a 7TM receptor and identify position II:20/2.60 as a generally important residue for ligand binding in certain 7TM receptors.


2012 ◽  
Vol 2012 ◽  
pp. 1-15 ◽  
Author(s):  
Ann-Sofie Mølleskov Jensen ◽  
Alexander Hovard Sparre-Ulrich ◽  
Nicholas Davis-Poynter ◽  
Mette Marie Rosenkilde

Several herpes- and poxviruses have captured chemokine receptors from their hosts and modified these to their own benefit. The human and viral chemokine receptors belong to class A 7 transmembrane (TM) receptors which are characterized by several structural motifs like the DRY-motif in TM3 and the C-terminal tail. In the DRY-motif, the arginine residue serves important purposes by being directly involved in G protein coupling. Interestingly, among the viral receptors there is a greater diversity in the DRY-motif compared to their endogenous receptor homologous. The C-terminal receptor tail constitutes another regulatory region that through a number of phosphorylation sites is involved in signaling, desensitization, and internalization. Also this region is more variable among virus-encoded 7TM receptors compared to human class A receptors. In this review we will focus on these two structural motifs and discuss their role in viral 7TM receptor signaling compared to their endogenous counterparts.


2011 ◽  
Vol 11 (6) ◽  
pp. 618-628 ◽  
Author(s):  
Kristine Norregaard ◽  
Tau Benned-Jensen ◽  
Mette Marie Rosenkilde
Keyword(s):  

Author(s):  
Jeffrey C. Jerman ◽  
Jason Brown ◽  
Magalie Rocheville

2010 ◽  
Vol 6 ◽  
pp. 33-47
Author(s):  
Adam I. Cygankiewicz

Seven-transmembrane (7TM) receptors are one of the most important proteins involved in perception of extracellular stimuli and regulation of variety of intracellular signaling pathways. Divergence of receptor types, their ligands and signaling pathways makes 7TM receptors important factors in pathology of many diseases. This review focused on the main diseases in which involvement of 7TM receptors was established e.g., retinitis pigmentosa, severe obesity, and dwarfism. Recent findings of aberrant expression of 7TM receptors in development of cancer were also summarized.


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