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• W2094993923 abstract "1 Endothelin (ET)-1 has been postulated to be involved in the development of obstructive airway diseases in man. In the present study, we attempted to characterize ET receptor subtypes mediating ET-1-induced contraction in human isolated bronchi. The ET receptor antagonists used in the present study were BQ-123 (ETA receptor-selective), BQ-788 (ETB receptor-selective) and BQ-928 (ETA/ETB dual). Sarafotoxin S6c (S6c) was also used as an ETB receptor-selective agonist. 2 In human bronchi, ET-1 and S6c (10−12 m to 10−7 M) produced concentration-dependent contraction with almost equal potency (pD2: 8.88± 0.16 for ET-1 and 9.42±0.15 for S6c). The contraction induced by S6c was competitively antagonized by BQ-788 alone (1 and 10 μm) with a pKB value of 7.49±0.21, suggesting that the stimulation of ETB receptors causes a contraction of human bronchi. However, contrary to expectation, the concentration-response curves for ET-1 were not affected by BQ-788. The ET-1- and S6c-induced contractions were not affected by BQ-123 (10 μm). Thus, ET-1-induced contraction of human bronchi is not antagonized by BQ-123 alone or by BQ-788 alone. 3 Combined treatment with 10 μm BQ-123 and 10 μm BQ-788 significantly antagonized the contraction induced by ET-1 with a dose-ratio of 11. BQ-928 also significantly antagonized ET-1-induced contraction with a pKB value of 6.32±0.24. 4The specific binding of [125I]-ET-1 to human bronchial membrane preparations was inhibited by BQ-123 (100 pM to 1 μm) by approximately 40%. Combination treatment with BQ-788 (100 pM to 1 μm) completely inhibited the BQ-123-resistant component of [125I]-ET-1 specific binding. 5 In conclusion, the present study demonstrates that BQ-788 alone cannot inhibit ET-1-induced contractions in human bronchi, although human bronchial ETB receptors are BQ-788-sensitive. Furthermore, it was shown that blockade of both receptor subtypes antagonizes ET-1-induced contraction, and that both receptor subtypes co-exist in human bronchial smooth muscles. These findings suggest that ETA receptors as well as ETB receptors are involved in ET-1-induced contraction in human bronchi. If ET-1 is involved in human airway diseases, dual blockade of ETA and ETB receptors may be necessary to treat the diseases." @default.
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• W2094993923 date "1996-03-01" @default.
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• W2094993923 title "Necessity of dual blockade of endothelin ETA and ETB receptor subtypes for antagonism of endothelin-1-induced contraction in human bronchi" @default.
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• W2094993923 doi "https://doi.org/10.1111/j.1476-5381.1996.tb16688.x" @default.
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