1999
DOI: 10.1074/jbc.274.18.12548
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Selective Modulation of Wild Type Receptor Functions by Mutants of G-Protein-coupled Receptors

Abstract: Members of the G-protein-coupled receptor (GPCR)family are involved in most aspects of higher eukaryote biology, and mutations in their coding sequence have been linked to several diseases. In the present study, we report that mutant GPCR can affect the functional properties of the co-expressed wild type (WT) receptor. Mutants of the human platelet-activating factor receptor that fail to show any detectable ligand binding (N285I and K298stop) or coupling to a G-protein (D63N, D289A, and Y293A) were co-expresse… Show more

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Cited by 54 publications
(31 citation statements)
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“…Our data are therefore consistent with the reported findings on the coexpression of N-terminal truncated, dominant-negative mutants and wild-type V 2 receptors, which results in the formation of heterodimers and reduced agonist binding, signal transduction, and cell-surface trafficking of the full-length V 2 receptor (Zhu and Wess, 1998). Similar to our findings on the 6TM-rH 3 isoforms, mutants of the ␣ 2 -AR (Zhou et al, 2006), vasopressin V 2 (Zhu and Wess, 1998), dopamine D 2 , chemokine receptor CCR5 (Benkirane et al, 1997;Blanpain et al, 2000;Chelli and Alizon, 2001), gonadotropinreleasing hormone receptor (Brothers et al, 2004), and the platelet-activating factor (Le Gouill et al, 1999) receptors also impede the cell surface expression of their coexpressed wild-type counterparts, thus exhibiting trans-dominant-negative effects on wild-type receptor expression (Benkirane et al, 1997;Chelli and Alizon, 2001;Brothers et al, 2004), most likely through dimerization. It seems most likely that the 6TM-rH 3 isoforms interfere with the functional expression of the 7TM-rH 3 Rs through heterodimerization.…”
Section: Discussionsupporting
confidence: 75%
“…Our data are therefore consistent with the reported findings on the coexpression of N-terminal truncated, dominant-negative mutants and wild-type V 2 receptors, which results in the formation of heterodimers and reduced agonist binding, signal transduction, and cell-surface trafficking of the full-length V 2 receptor (Zhu and Wess, 1998). Similar to our findings on the 6TM-rH 3 isoforms, mutants of the ␣ 2 -AR (Zhou et al, 2006), vasopressin V 2 (Zhu and Wess, 1998), dopamine D 2 , chemokine receptor CCR5 (Benkirane et al, 1997;Blanpain et al, 2000;Chelli and Alizon, 2001), gonadotropinreleasing hormone receptor (Brothers et al, 2004), and the platelet-activating factor (Le Gouill et al, 1999) receptors also impede the cell surface expression of their coexpressed wild-type counterparts, thus exhibiting trans-dominant-negative effects on wild-type receptor expression (Benkirane et al, 1997;Chelli and Alizon, 2001;Brothers et al, 2004), most likely through dimerization. It seems most likely that the 6TM-rH 3 isoforms interfere with the functional expression of the 7TM-rH 3 Rs through heterodimerization.…”
Section: Discussionsupporting
confidence: 75%
“…This is suggested by evidence that the trafficking of wild-type receptors to the cell surface can be inhibited by mutants (e.g. Le Gouill et al 1999;Zhu and Wess 1998); also, the transfer of resonance energy between tagged receptors can be detected in membrane fractions enriched in endoplasmic reticulum (Terrillon et al 2003). It follows that the oligomeric status of the receptor is established early on and therefore is expected to be the same regardless of whether the receptor is localized intracellularly or at the plasma membrane.…”
Section: Discussionmentioning
confidence: 89%
“…1) The mutant receptor does not affect wild type signaling; 2) the mutant receptor inhibits wild type signaling either by inhibiting surface expression or the activation of signaling (8 -10); or 3) the wild type receptor can functionally rescue the mutant receptor (11,12,37). In addition, co-expression of two nonfunctional receptors can create functional receptors (17,38).…”
Section: Co-expression Of Mutant Receptors and Wild Type Inhibit G␣ Qmentioning
confidence: 99%