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人补体蛋白C8β亚基的互补DNA及推导的氨基酸序列:与α亚基和C9的紧密结构及祖先关系的鉴定

Complementary DNA and derived amino acid sequence of the beta subunit of human complement protein C8: identification of a close structural and ancestral relationship to the alpha subunit and C9.

作者信息

Howard O M, Rao A G, Sodetz J M

机构信息

Department of Chemistry and School of Medicine, University of South Carolina, Columbia 29208.

出版信息

Biochemistry. 1987 Jun 16;26(12):3565-70. doi: 10.1021/bi00386a047.

DOI:10.1021/bi00386a047
PMID:2820472
Abstract

A cDNA clone encoding the beta subunit (Mr 64,000) of the eighth component of complement (C8) has been isolated from a human liver cDNA library. This clone has a cDNA insert of 1.95 kilobases (kb) and contains the entire beta sequence [1608 base pairs (bp)]. Analysis of total cellular RNA isolated from the hepatoma cell line HepG2 revealed the mRNA for beta to be approximately 2.5 kb. This is similar to the message size for the alpha subunit of C8 and confirms the existence of different mRNAs for alpha and beta. This finding supports genetic evidence that alpha and beta are encoded at different loci. Analysis of the derived amino acid sequence revealed several membrane surface seeking segments that may facilitate beta interaction with target membranes during complement-mediated cytolysis. Determination of the carbohydrate composition indicated 1 or 2 asparagine-linked but no O-linked oligosaccharide chains. Comparison of the beta sequence to that reported for alpha in the preceding paper [Rao, A. G., Howard, O. M. Z., Ng, S. C., Whitehead, A. S., Colten, H. R. & Sodetz, J. M. (1987) Biochemistry (preceding paper in this issue)] and to that of human C9 revealed a striking homology between all three proteins. For beta and alpha, the overall homology is 33% on the basis of identity and 53% when conserved substitutions are allowed. For beta and C9, the values are 26% and 47%, respectively.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

已从人肝cDNA文库中分离出一个编码补体第八成分(C8)β亚基(分子量64,000)的cDNA克隆。该克隆的cDNA插入片段为1.95千碱基(kb),包含完整的β序列[1608个碱基对(bp)]。对从肝癌细胞系HepG2分离的总细胞RNA的分析显示,β的mRNA约为2.5 kb。这与C8α亚基的信息大小相似,并证实了α和β存在不同的mRNA。这一发现支持了α和β在不同基因座编码的遗传学证据。对推导的氨基酸序列的分析揭示了几个可能有助于β在补体介导的细胞溶解过程中与靶膜相互作用的膜表面寻找片段。碳水化合物组成的测定表明有1或2条天冬酰胺连接的寡糖链,但没有O连接的寡糖链。将β序列与前一篇论文[Rao, A. G., Howard, O. M. Z., Ng, S. C., Whitehead, A. S., Colten, H. R. & Sodetz, J. M. (1987) Biochemistry(本期前一篇论文)]中报道的α序列以及人C9的序列进行比较,发现这三种蛋白质之间有显著的同源性。对于β和α,基于同一性的总体同源性为33%,允许保守替换时为53%。对于β和C9,相应的值分别为26%和47%。(摘要截短于250字)

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