| 家族性高胆固醇血症家系低密度脂蛋白受体基因剪接突变的研究 |
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| 引用本文: | 蔺洁,王绿娅,刘舒,潘晓冬,杜兰平,石凤茹,秦彦文,赵庆,郭恒怡. 家族性高胆固醇血症家系低密度脂蛋白受体基因剪接突变的研究[J]. 中华医学遗传学杂志, 2004, 21(1): 14-18 |
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| 作者姓名: | 蔺洁 王绿娅 刘舒 潘晓冬 杜兰平 石凤茹 秦彦文 赵庆 郭恒怡 |
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| 作者单位: | 1. 100029,北京市心肺血管疾病研究所-首都医科大学附属北京安贞医院动脉硬化研究室
2. 中国医学科学院基础医学研究所 |
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| 基金项目: | 北京市自然科学基金 (70 32 0 1 2 ),首都医科大学基础临床合作基金 (0 2 JL1 9)~~ |
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| 摘 要: | 目的 检测中国汉族家族性高胆固醇血症 (familial hypercholesterolemia,FH)大家系低密度脂蛋白受体 (low density lipoprotein receptor,L DL R)基因突变 ,探讨 FH发病的分子机理。方法 首先采用聚合酶链反应 -限制性片段长度多态性 (polymerase chain reaction- restriction fragment lengthpolymorphism,PCR- RFL P)技术检测载脂蛋白 B1 0 0 (apo B1 0 0 )基因 Q35 0 0 R突变 ,排除家族性 apo B1 0 0 缺陷症 ,再采用 PCR扩增结合核苷酸序列分析检测 1例临床诊断为 FH纯合子患儿及其家系成员 L DL R基因启动子和全部 18个外显子片段 ,结果与 Gen Bank公布的该基因正常序列对比找出突变 ,并在家系其他成员中证实该突变。结果 该患儿 L DL R基因第 3内含子剪接供体处存在 IN 5′GT→AT纯合剪接突变 ,并且在家系中得到证实 ,一级和二级亲属中各发现 2例相同位点和相同形式的杂合子 ,其基因型表现为野生型和突变型杂合现象。同时未检测出患儿及其父母 apo B1 0 0 Q35 0 0 R突变。结论 发现 L DL R基因第 3内含子 G→ A纯合剪接突变 ,可能是该 FH家系发病的分子基础 ;检测该突变对临床干预和遗传指导有参考价值。
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| 关 键 词: | 家族性高胆固醇血症 低密度脂蛋白受体 剪接突变 |
| 修稿时间: | 2003-07-24 |
Identification of a novel splice mutation of low density lipoprotein receptor gene in a Chinese family with familial hypercholesterolemia |
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| LIN Jie ,WANG Lu-ya ,LIU Shu ,PAN Xiao-dong ,DU Lan-ping ,SHI Feng-ru ,QIN Yan-wen ,ZHAO Qing ,GUO Heng-yi .. Identification of a novel splice mutation of low density lipoprotein receptor gene in a Chinese family with familial hypercholesterolemia[J]. Chinese journal of medical genetics, 2004, 21(1): 14-18 |
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| Authors: | LIN Jie WANG Lu-ya LIU Shu PAN Xiao-dong DU Lan-ping SHI Feng-ru QIN Yan-wen ZHAO Qing GUO Heng-yi . |
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| Affiliation: | Beijing Institute of Heart Lung and Blood Vessel Diseases, Beijing, PR China. linjie1998@sina.com.cn |
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| Abstract: | OBJECTIVE: To identify the mutation of low density lipoprotein receptor(LDLR) gene in a large Chinese family with familial hypercholesterolemia(F H) and make a discussion on the pathogenesis of FH at the molecular level. METHODS: Investigations were made on a patient with the clinical phenotype of homozygous FH and his parents for mutations of promoter and all 18 exons of LDLR gene. Screening was carried out using Touch down PCR and a g arose gel electrophoresis, combined with DNA sequence analysis. The results were compared with the normal sequences in GenBank and FH database (www.ucl.uk/fh) t o find the mutation. Then the mutation was identified in other members of the family. In addition, the authors screened the apolipoprotein B(100) (apoB(100)) gene f or known mutations (R3500Q) that cause familial defective apoB(100) (FDB) by PCR-RFLP. RESULTS: A novel homozygous IN III 5' GT --> AT mutation in the splice donor of LDLR intron 3 was detected in the homozygote propositus with FH. The mutation was also identified in four heterozygous carriers in his family. No mutations R3500Q of apoB(100)were observed. CONCLUSION: A homozygous G --> A splice mutation in LDLR gene was first reported. The change of the splice donor in LDLR intron 3 may cause skipping of exon 3, which is responsible for FH. Perhaps it is a particular pathogenesis for Chinese people. |
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| Keywords: | familial hypercholesterolemia low density lipoprotein receptors splice mutation |
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