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Role of the hexapeptide disulfide loop in the gamma-carboxyglutamic acid domain of protein C in Ca2+-mediated structural and functional properties

机译:六肽二硫键环在C2介导的结构和功能特性中的蛋白C的γ-羧基谷氨酸结构域中的作用

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摘要

The anticoagulant and immunomodulatory effects of protein C (PC) rely on the presence of the N-terminal gamma-carboxyglutamic acid (Gla) domain. This domain is strongly conserved among vitamin K-dependent blood proteins and, in addition to a high relative content of Gla, contains a hexapeptide disulfide loop between Cys residues 17 and 22. In the present study, the contribution of the hexapeptide loop toward Gla domain structure and function was evaluated using wild-type and Cys17/Cys22-alkylated synthetic peptide analogues of the 47-residue Gla domain/helical stack of PC. Circular dichroism and intrinsic fluorescence measurements revealed significant differences in the metal ion-dependent conformations of the two peptides. Disruption of the disulfide loop slightly altered the capacity of the peptide to interact with acidic phospholipid (PL) vesicles. The affinity of the alkylated peptide for soluble endothelial protein C receptor (EPCR), as demonstrated by surface plasmon resonance studies, was increased compared with the wild-type species, although total binding was compromised. These results suggest that the disulfide loop of PC contributes to the overall Ca2+-dependent conformation but is not strictly required for PL membrane binding or EPCR recognition.
机译:蛋白C(PC)的抗凝血和免疫调节作用依赖于N末端γ-羧基谷氨酸(Gla)域的存在。该结构域在维生素K依赖的血液蛋白中高度保守,除了高含量的Gla外,还包含Cys残基17和22之间的六肽二硫键。在本研究中,六肽环对Gla域的贡献使用野生型和PCS螺旋残基的47个残基的Cys17 / Cys22烷基化的合成肽类似物评估结构和功能。圆二色性和固有荧光测量结果表明,两种肽的金属离子依赖性构象存在显着差异。二硫键环的破坏稍微改变了肽与酸性磷脂(PL)囊泡相互作用的能力。表面等离振子共振研究表明,烷基化肽对可溶性内皮蛋白C受体(EPCR)的亲和力与野生型相比有所提高,尽管总结合受到了损害。这些结果表明PC的二硫键环有助于整体的Ca2 +依赖性构象,但对于PL膜结合或EPCR识别并不是严格要求的。

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