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人类补体成分C6的分子结构

The molecular architecture of human complement component C6.

作者信息

DiScipio R G, Hugli T E

机构信息

Research Institute of Scripps Clinic, La Jolla, California 92037.

出版信息

J Biol Chem. 1989 Sep 25;264(27):16197-206.

PMID:2789218
Abstract

The molecular architecture of human complement component C6 was elucidated at several levels of structural organization. The entire primary structure of C6 was determined by sequencing C6 cDNA that was cloned from a human liver lambda gt11 library. The polypeptide chain of C6 contains 913 amino acids. The protein is homologous with the other terminal components of complement, C7-C9. Specifically, C6 has 29% of its residues identical with C7, and 55 of the 56 cysteines found in C7 match those in C6. The C6 polypeptide chain is cross-linked by 32 disulfide bonds, and most of the cysteines are located in short (34-77 amino acids) discrete segments that exhibit homology with a wide variety of other proteins such as thrombospondin, the low density lipoprotein receptor, epidermal growth factor, and complement factors H and I. C6 is a glycoprotein, and it has two oligosaccharide groups attached to asparagines located near the amino and the carboxyl termini of the molecule. The organization of secondary structural elements in C6 was elucidated using circular dichroism spectroscopy and an empirical method based on sequence analysis. C6 has an estimated 12% alpha-helix, but is comparatively richer in beta-sheet (29%) and beta-turns (21%). Most of the predicted alpha-helical structure resides in a portion of the polypeptide chain that is free of cysteine and which shares homology with C9 and perforin. The tertiary structure of the C6 molecule was visualized by transmission electron microscopy; it has a sickle shape with dimensions of 144 x 66 A. The combined results are discussed and comparisons made with the other late acting components of complement and perforin.

摘要

人类补体成分C6的分子结构在多个结构组织层面得到了阐明。通过对从人肝λgt11文库中克隆的C6 cDNA进行测序,确定了C6的完整一级结构。C6的多肽链包含913个氨基酸。该蛋白质与补体的其他末端成分C7 - C9具有同源性。具体而言,C6有29%的残基与C7相同,C7中发现的56个半胱氨酸中有55个与C6中的半胱氨酸匹配。C6多肽链通过32个二硫键交联,大多数半胱氨酸位于短的(34 - 77个氨基酸)离散片段中,这些片段与多种其他蛋白质具有同源性,如血小板反应蛋白、低密度脂蛋白受体、表皮生长因子以及补体因子H和I。C6是一种糖蛋白,它有两个寡糖基团连接在靠近分子氨基和羧基末端的天冬酰胺上。利用圆二色光谱和基于序列分析的经验方法阐明了C6中二级结构元件的组织情况。C6估计有12%的α - 螺旋,但β - 折叠(29%)和β - 转角(21%)相对更丰富。大多数预测的α - 螺旋结构存在于多肽链中不含半胱氨酸且与C9和穿孔素具有同源性的部分。通过透射电子显微镜观察到C6分子的三级结构;它呈镰刀状,尺寸为144×66埃。讨论了综合结果,并与补体的其他后期作用成分和穿孔素进行了比较。

相似文献

1
The molecular architecture of human complement component C6.人类补体成分C6的分子结构
J Biol Chem. 1989 Sep 25;264(27):16197-206.
2
The structure of human complement component C7 and the C5b-7 complex.人类补体成分C7及C5b-7复合物的结构。
J Biol Chem. 1988 Jan 5;263(1):549-60.
3
Complete primary structure and functional characterization of the sixth component of the human complement system. Identification of the C5b-binding domain in complement C6.人类补体系统第六成分的完整一级结构及功能特性。补体C6中C5b结合结构域的鉴定。
J Biol Chem. 1989 Oct 25;264(30):18041-51.
4
Structural homology of complement protein C6 with other channel-forming proteins of complement.补体蛋白C6与补体其他形成通道蛋白的结构同源性。
Proc Natl Acad Sci U S A. 1989 Apr;86(8):2799-803. doi: 10.1073/pnas.86.8.2799.
5
Cloning, analysis, and expression of murine perforin 1 cDNA, a component of cytolytic T-cell granules with homology to complement component C9.小鼠穿孔素1 cDNA的克隆、分析及表达,穿孔素1是细胞毒性T细胞颗粒的一个成分,与补体成分C9具有同源性。
Proc Natl Acad Sci U S A. 1989 Jan;86(1):247-51. doi: 10.1073/pnas.86.1.247.
6
Phylogenetic analysis of the homologous proteins of the terminal complement complex supports the emergence of C6 and C7 followed by C8 and C9.末端补体复合物同源蛋白的系统发育分析支持C6和C7先出现,随后是C8和C9。
J Mol Evol. 1999 Aug;49(2):282-9. doi: 10.1007/pl00006550.
7
Structure of the human C7 gene and comparison with the C6, C8A, C8B, and C9 genes.人类C7基因的结构及其与C6、C8A、C8B和C9基因的比较。
J Immunol. 1995 May 15;154(10):5188-94.
8
Structural/functional similarity between proteins involved in complement- and cytotoxic T-lymphocyte-mediated cytolysis.补体和细胞毒性T淋巴细胞介导的细胞溶解相关蛋白之间的结构/功能相似性。
Nature. 1986;322(6082):831-4. doi: 10.1038/322831a0.
9
Homology of perforin to the ninth component of complement (C9).穿孔素与补体第九成分(C9)的同源性。
Nature. 1988 Aug 11;334(6182):525-7. doi: 10.1038/334525a0.
10
The heparin binding domain of S-protein/vitronectin binds to complement components C7, C8, and C9 and perforin from cytolytic T-cells and inhibits their lytic activities.S 蛋白/玻连蛋白的肝素结合结构域与补体成分 C7、C8 和 C9 以及细胞毒性 T 细胞的穿孔素结合,并抑制它们的溶解活性。
Biochemistry. 1988 May 31;27(11):4103-9. doi: 10.1021/bi00411a029.

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