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C3a过敏毒素的活性位点:亲脂性和定向残基的作用

Active site of C3a anaphylatoxin: contributions of the lipophilic and orienting residues.

作者信息

Unson C G, Erickson B W, Hugli T E

出版信息

Biochemistry. 1984 Feb 14;23(4):585-9. doi: 10.1021/bi00299a001.

Abstract

Activation of the serum complement cascade generates C3a anaphylatoxin, a primary mediator of inflammation. The active-site pentapeptide from the COOH terminus of C3a, Leu-Gly-Leu-Ala-Arg (residues 73-77), exhibits the inflammatory activities and specificity of the native 77-residue polypeptide. Functionally important features of this active site were studied by testing the ability of 22 synthetic analogues of this pentapeptide to contract isolated muscle strips from guinea pig ileum and to desensitize this tissue to contraction induced by human C3a or C5a. The C3a receptors on mast cells and basophils probably contain lipophilic groups that interact with the lipophilic side chains of Leu-73 and Leu-75 and charged groups that interact with the carboxylate and guanidinium groups of Arg-77. The lipophilic contribution of Leu-73 is modest and sterically nonspecific while that of Leu-75 is substantial and sterically specific. Gly-74 and Ala-76 appear to position and orient the adjacent residues Leu-73, Leu-75, and Arg-77 for optimal receptor binding. The contribution of Gly-74 is neither conformationally nor sterically specific while that of Ala-76 is both conformationally and sterically specific. The cellular C3a receptors evidently interact most efficiently with peptides ending in -Leu-Ala-Arg-OH.

摘要

血清补体级联反应的激活会产生C3a过敏毒素,这是炎症的主要介质。来自C3a羧基末端的活性位点五肽Leu-Gly-Leu-Ala-Arg(残基73 - 77)表现出天然77个残基多肽的炎症活性和特异性。通过测试该五肽的22种合成类似物使豚鼠回肠离体肌肉条收缩以及使该组织对人C3a或C5a诱导的收缩脱敏的能力,研究了这个活性位点的功能重要特征。肥大细胞和嗜碱性粒细胞上的C3a受体可能含有与Leu-73和Leu-75的亲脂性侧链相互作用的亲脂性基团,以及与Arg-77的羧酸盐和胍基相互作用的带电基团。Leu-73的亲脂性贡献适中且空间上无特异性,而Leu-75的贡献显著且空间上有特异性。Gly-74和Ala-76似乎将相邻残基Leu-73、Leu-75和Arg-77定位并定向以实现最佳受体结合。Gly-74的贡献在构象和空间上均无特异性,而Ala-76的贡献在构象和空间上均有特异性。细胞C3a受体显然与以-Leu-Ala-Arg-OH结尾的肽相互作用最为有效。

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