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Binding of synthetic beta-human atrial natriuretic peptide to cultured rat vascular smooth muscle cells.

作者信息

Hirata Y, Yoshimi H, Takata S, Matsubara H, Takagi Y, Iida T, Chino N, Watanabe T X, Kimura T, Sakakibara S

出版信息

FEBS Lett. 1987 Jul 27;219(2):369-74. doi: 10.1016/0014-5793(87)80255-7.

DOI:10.1016/0014-5793(87)80255-7
PMID:3038609
Abstract

We have studied the effects of synthetic beta-human atrial natriuretic peptide (beta-hANP), an antiparallel dimer of alpha-hANP, on receptor binding and cGMP generation in cultured rat vascular smooth muscle cells and compared the effects with those of alpha-hANP. Characteristics of temperature-dependent binding and degradation of 125I-beta-hANP were similar to those of 125I-alpha-hANP. Scatchard analysis indicated a single class of binding sites for beta-hANP with a maximal binding capacity one-half that of alpha-hANP. Parallel and antiparallel dimers were equipotent in inhibiting the binding and stimulating intracellular cGMP formation, of which the maximal effect was about one-half that of alpha-hANP. Reverse-phase high performance liquid chromatography revealed that most of beta-hANP added to cells was converted to a small molecular mass component corresponding to alpha-hANP after incubation. These data suggest that the less potent effect of beta-hANP in receptor binding and cGMP generation may be partly accounted for by the possible conversion of beta-hANP to alpha-hANP at the site of target cells.

摘要

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