Synthesis and Biological Property of α-Human Atrial Natriuretic Peptide Analogs with a Constrained or Stereochemically Modified Cyclic Moiety
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概要
- 論文の詳細を見る
Conformationally restricted analogs of α-human atrial natriuretic peptide (α-hANP) containing L- or D-penicillamine, or D-cysteine in place of cysteine residues at positions 7 and 23 were synthesized by the liquid phase procedure. Their biological properties in the assays of receptor binding and cyclic guanosine monophosphate (cGMP) accumulation employing rat vascular smooth muscle cells (VSMC), vasorelaxant activity using rat isolated aorta were evaluated. We found that the constrained and/or stereochemically altered ring moiety generally did not influence the receptor binding activity, however, cGMP accumulation and vasorelaxant activities were quite sensitive to conformational perturbation. Furthermore, a lack of correlation between cGMP acccumulation activity and vasorelaxant activity was observed. Dissociation between these activities was typical in the case of [^DPen^<7,23>]-α-hANP(7-28), which showed quite weak vasorelaxant activity in spite of its full cGMP accumulation and receptor binding potencies. This result suggests that cGMP accumulation alone is not sufficient to promote AMP-induced vasorelaxation, and that the other second messenger (s) may mediate this activity.
- 社団法人日本薬学会の論文
- 1990-07-25
著者
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古谷 真優美
サントリー生物医学研究所
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田中 正治
サントリー・生医研
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南竹 義春
Suntory Institute for Biomedical Research
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北島 安雄
Suntory Institute for Biomedical Research
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古谷 真優美
Suntory Institute for Biomedical Research
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田中 正治
Suntory Institute for Biomedical Research
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武久 真己
Suntory Institute for Biomedical Research
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