Mutations in the B-2 bradykinin receptor reveal a different pattern of contacts for peptidic agonists and peptidic antagonists

被引:62
作者
Jarnagin, K
Bhakta, S
Zuppan, P
Yee, C
Ho, T
Phan, T
Tahilramani, R
Pease, JHB
Miller, A
Freedman, R
机构
[1] ROCHE BIOSCI,MED CHEM,PALO ALTO,CA 94304
[2] ROCHE BIOSCI,MOL STRUCT GRP,INFLAMMATORY DIS UNIT,PALO ALTO,CA 94304
关键词
D O I
10.1074/jbc.271.45.28277
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
The B-2 bradykinin receptor, a seven-helix transmembrane receptor, binds the inflammatory mediator bradykinin (BK) and the structurally related peptide antagonist HOE-140, The binding of HOE-140 and the binding of bradykinin are mutually exclusive and competitive. Fifty-four site-specific receptor mutations were made, BK's affinity is reduced 2200-fold by F261A, 490-fold by T265A, 60-fold by D286A, and 3-10-fold by N200A, D268A, and Q290A, In contrast, HOE-140 affinity is reduced less than 7-fold by F254A, F261A, Y297A, and Q262A. The almost complete discordance of mutations that affect BK binding versus HOE-140 binding is surprising, but it was paralleled by the effect of single changes in BK and HOE-140. [Ala(9)]BK and [Ala(6)]BK are reduced in receptor binding affinity 27,000- and 150-fold, respectively, while [Ala(9)]HOE-140 affinity is reduced 7-fold and [Ala(6)]HOE-140 affinity is unchanged. NMR spectroscopy of all of the peptidic analogs of BK or HOE-140 revealed a beta-turn at the C terminus. Models of the receptor-ligand complex suggested that bradykinin is bound partially inside the helical bundle of the receptor with the amino terminus emerging from the extracellular side of helical bundle, In these models a salt bridge occurs between Arg(9) and Asp(286); the models also place Phe(8) in a hydrophobic pocket midway through the transmembrane region. Models of HOE-140 binding to the receptor place its beta-turn one alpha-helical turn deeper and closer to helix 7 and helix 1 as compared with bradykinin-receptor complex models.
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页码:28277 / 28286
页数:10
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