Residues 293 and 294 are ligand contact points of the human angiotensin type 1 receptor

Autor: Mannix Auger-Messier, Jacqueline Pérodin, Maud Deraët, Antony A. Boucard, Jean-Luc Parent, Richard Leduc, Marie-Eve Beaulieu, Pierre Lavigne, Emanuel Escher, Lenka Rihakova, Gaétan Guillemette
Rok vydání: 2002
Předmět:
Zdroj: Biochemistry. 41(48)
ISSN: 0006-2960
Popis: The human angiotensin II type 1 receptor (hAT 1 ) was photolabeled with a high-affinity radiolabeled photoreactive analogue of AngII, 1 2 5 I-[Sar 1 , Val 5 , p-Benzoyl-L-phenylalanine 8 ]AngII ( 1 2 5 I-[Sar 1 ,Bpa 8 ]AngII). Chemical cleavage with CNBr produced a 7 kDa fragment (285-334) of the C-terminal portion of the hAT 1 . Manual Edman radiosequencing of photolabeled, per-acetylated, and CNBr-fragmented receptor showed that ligand incorporation occurred through Phe 2 9 3 and Asn 2 9 4 within the seventh transmembrane domain of the hAT 1 . Receptor mutants with Met introduced at the presumed contact residues, F293M and N294M, were photolabeled and then digested with CNBr. SDS-PAGE analysis of those digested mutant receptors confirmed the contact positions 293 and 294 through ligand release induced by CNBr digestion. Additional receptor mutants with Met residues introduced into the N- and C-terminal proximity of those residues 293 and 294 of the hAT 1 produced, upon photolabeling and CNBr digestion, fragmentation patterns compatible only with the above contact residues. These data indicate that the C-terminal residue of AngII interacts with residues 293 and 294 of the seventh transmembrane domain of the human AT 1 receptor. Taking into account a second receptor-ligand contact at the second extracellular loop and residue 3 of AngII (Boucard, A. A., Wilkes, B. C., Laporte, S. A., Escher, E., Guillemette, G., and Leduc, R. (2000) Biochemistry 39, 9662-70) the Ang II molecule must adopt an extended structure in the AngII binding pocket.
Databáze: OpenAIRE
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