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人肝脏载脂蛋白B - 100 cDNA:完整核酸序列及推导的氨基酸序列

Human liver apolipoprotein B-100 cDNA: complete nucleic acid and derived amino acid sequence.

作者信息

Law S W, Grant S M, Higuchi K, Hospattankar A, Lackner K, Lee N, Brewer H B

出版信息

Proc Natl Acad Sci U S A. 1986 Nov;83(21):8142-6. doi: 10.1073/pnas.83.21.8142.

Abstract

Human apolipoprotein B-100 (apoB-100), the ligand on low density lipoproteins that interacts with the low density lipoprotein receptor and initiates receptor-mediated endocytosis and low density lipoprotein catabolism, has been cloned, and the complete nucleic acid and derived amino acid sequences have been determined. ApoB-100 cDNAs were isolated from normal human liver cDNA libraries utilizing immunoscreening as well as filter hybridization with radiolabeled apoB-100 oligodeoxynucleotides. The apoB-100 mRNA is 14.1 kilobases long encoding a mature apoB-100 protein of 4536 amino acids with a calculated amino acid molecular weight of 512,723. ApoB-100 contains 20 potential glycosylation sites, and 12 of a total of 25 cysteine residues are located in the amino-terminal region of the apolipoprotein providing a potential globular structure of the amino terminus of the protein. ApoB-100 contains relatively few regions of amphipathic helices, but compared to other human apolipoproteins it is enriched in beta-structure. The delineation of the entire human apoB-100 sequence will now permit a detailed analysis of the conformation of the protein, the low density lipoprotein receptor binding domain(s), and the structural relationship between apoB-100 and apoB-48 and will provide the basis for the study of genetic defects in apoB-100 in patients with dyslipoproteinemias.

摘要

人载脂蛋白B-100(apoB-100)是低密度脂蛋白上与低密度脂蛋白受体相互作用并启动受体介导的内吞作用和低密度脂蛋白分解代谢的配体,已被克隆,其完整的核酸和推导的氨基酸序列也已确定。利用免疫筛选以及与放射性标记的apoB-100寡脱氧核苷酸进行滤膜杂交,从正常人肝脏cDNA文库中分离出apoB-100 cDNA。apoB-100 mRNA长14.1千碱基,编码一个由4536个氨基酸组成的成熟apoB-100蛋白,计算得到的氨基酸分子量为512,723。apoB-100含有20个潜在的糖基化位点,在总共25个半胱氨酸残基中,有12个位于载脂蛋白的氨基末端区域,这为该蛋白氨基末端提供了潜在的球状结构。apoB-100含有的两亲性螺旋区域相对较少,但与其他人类载脂蛋白相比,它富含β结构。完整的人apoB-100序列的描绘现在将允许对该蛋白的构象、低密度脂蛋白受体结合结构域以及apoB-100与apoB-48之间的结构关系进行详细分析,并将为研究血脂异常患者apoB-

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