Polar residues in the transmembrane domains of the type 1 angiotensin II receptor are required for binding and coupling - Reconstitution of the binding site by co-expression of two deficient mutants

被引:191
作者
Monnot, C
Bihoreau, C
Conchon, S
Curnow, KM
Corvol, P
Clauser, E
机构
[1] INSERM, College de France, 75005 Paris, 3, rue d'Ulm
关键词
D O I
10.1074/jbc.271.3.1507
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Type 1 angitensin receptors (AT(1)) are G protein coupled receptors, mediating the physiological actions of the vasoactive peptide ansotensin II, In this study, the roles of 7 amino acids of the rat AT(1A) receptor in ligand binding and signaling were investigated by performing functional assays of individual receptor mutants expressed in COS and Chinese hamster ovary cells, Substitutions of polar residues in the third transmembrane domain with Ala indicate that Ser(105), Ser(107), and Ser(109) are not essential for maintenance of the ansotensin II binding site, Replacement of Asn(111) or Ser(115) does not alter the binding affinity for peptidic analogs, but modifies the ability of the receptor to interact with AT, (DuP753)- or AT(2) (CGP42112A)-specific ligands, These 2 residues are probably involved in determining the binding specificity for these analogs, The absence of G-protein coupling to the Ser(115) mutant suggests that this residue, in addition to previously identified residues, Asp(74) and Tyr(292), participates in the receptor activation mechanism. Finally, Lys(102) (third helix) and Lys(199) (fifth helix) mutants do not bind angiotensin II or different analogs, Go-expression of these two deficient receptors permitted the restoration of a normal binding site, This effect was not due to homologous recombination of the cDNAs but to protein trans complementation.
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页码:1507 / 1513
页数:7
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