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载脂蛋白B-100受体结合缺陷新变种的检测
引用本文:Li Y,Feng J,Li W. 载脂蛋白B-100受体结合缺陷新变种的检测[J]. 中华医学杂志, 2001, 81(23): 1434-1435
作者姓名:Li Y  Feng J  Li W
作者单位:1. 新加坡国立大学
2. 暨南大学医学院生化教研室
3. 珠海市妇幼保健院
基金项目:国家自然科学基金资助项目(39570391)
摘    要:目的:筛查导致家族性载脂蛋白B-100(apoB-100)受体结合缺陷的未知突变,以阐明高胆固醇血症的遗传背景,了解apoB-100受体结合区的定位。方法:以原发性高胆固醇血症患者为对象,用聚合酶链反应(PCR)扩增apoB基因第26外显子编码2980-3084位氨基酸残基的核苷酸序列,长363碱基对,产物进行单链构像多态性(SSCP)分析,以筛查可能存在的突变。结果:341例样本的SSCP图像均未发现异常电泳带。结论:(1)广东原发性高胆固醇血症患者上述区段不存在突变,或突变率很低;(2)不支持2980-3084残基是apoB-100的受体结合区的假说。

关 键 词:载脂蛋白B 高胆固醇血症 单链构像多态性 家族性 apoB-100缺陷症 FDB
修稿时间:2001-03-28

Screening for the new variant of defective receptor-binding apolipoprotein B-100
Li Y,Feng J,Li W. Screening for the new variant of defective receptor-binding apolipoprotein B-100[J]. Zhonghua yi xue za zhi, 2001, 81(23): 1434-1435
Authors:Li Y  Feng J  Li W
Affiliation:Department of Biochemistry, Medical College of Jinan University, Guangzhou 510632, China.
Abstract:OBJECTIVE: To detect possibly existing unknown mutation(s) in nucleotide sequence coding amino acid residues 2,980 to 3,084, that may lead to familial defective apo B-100, and to provide evidence for evaluating the putative receptor binding domain of apo B-100. METHODS: The nucleotide sequence coding the amino acid resudues 2,980-3,084 of apo B gene in 341 patients with primary hypercholesteremia and of 50 controls was amplified by PCR and subjected to single strand conformational polymorphism analysis under optimized conditions. RESULTS: No abnormal electrophoretic figure was found in the samples from 341 hypercholesterlemic patients and 50 controls. CONCLUSION: (1) Point mutation causing hypercholesterlemia is unlikely to exist, or rare, if any, in the codons 2,980-3,084 of apo B-100 in Chinese. (2) Amino acid residues 2,980-3,084 may not be involved in the receptor-binding of apo B-100.
Keywords:Apolipoprotein B  Genetic disease  Hypercholesterlemia  Single strand conformational polymorphism
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