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NKX2—5基因与先天性心脏病的关系
引用本文:刘兴元,杨奕清,杨颖,林小平,陈义汉. NKX2—5基因与先天性心脏病的关系[J]. 国外医学:心血管疾病分册, 2009, 0(4): 232-235
作者姓名:刘兴元  杨奕清  杨颖  林小平  陈义汉
作者单位:上海同济大学附属同济医院儿科;上海同济大学附属同济医院心内科;同济大学医学遗传研究所;
基金项目:国家杰出青年科学基金(30425016); 国家自然科学基金(30570768); 海外青年学者合作研究基金(30528011); 上海市优秀学科带头人计划项目(05XD14014)
摘    要:目的:探讨NKX2—5基因与先天性心脏病(congenital heart disease,CHD)的关系。方法:收集130例无血缘关系的CHD患者的临床资料和血标本,以100名无血缘关系的健康者为对照。应用聚合酶链反应扩增CHD候选基因NKX2—5的全部外显子和外显子两侧的部分内含子,采用双脱氧核苷链末端合成终止法对全部扩增片段进行测序。将所测的序列与GenBank数据库中公布的NKX2—5基因序列进行比对以识别出NKX2—5基因变异。比较识别出的NKX2—5基因多态在CHD患者和健康对照者间的频率分布差异。结果:在CHD患者的NKX2—5基因识别出2个单核苷酸多态,一个是NKx2—5基因编码序列第63位的腺嘌呤(A)变为鸟嘌呤(G),即c.63A〉G多态;另一个是NKx2—5基因编码序列第606位的G变为胞嘧啶(C),即c.606G〉C多态。在NKX2—5基因第606位点的等位基因G、C及其构成的3种基因型GG、GC、CC在CHD患者和健康对照者间的频率分布有显著性差异(等位基因频率比较:X^2=4.125,P=0.042;基因型频率比较:X^2=4.279,P=0.039)。但在NKX2—5基因第63位点的等位基因A、G及其构成的3种基因型AA、AG、GG在CHD患者和健康对照者间的频率分布无显著性差异(等位基因频率比较:X^2=0.704,P=0.402;基因型频率比较:X^2=0.626,P=0.429)。结论:NKX2—5基因c.606G〉C多态可能与CHD有关,等位基因606C携带者可能对CHD的易感性增加。

关 键 词:先天性心脏病  遗传学  NKX2—5  转录调节

Association of NKX2-5 gene with congenital heart disease
LIU Xing-yuan,YANG Yi-qing,YANG Ying,LIN Xiao-ping,CHEN Yi-han.. Association of NKX2-5 gene with congenital heart disease[J]. , 2009, 0(4): 232-235
Authors:LIU Xing-yuan  YANG Yi-qing  YANG Ying  LIN Xiao-ping  CHEN Yi-han.
Affiliation:LIU Xing-yuan1,YANG Yi-qing2,YANG Ying2,LIN Xiao-ping2,CHEN Yi-han2. 1. Department of Paediatrics,Tongji University Affiliated Tongji Hospital,Shanghai 200065,China,2. Department of Cardiology,Tongji University Affiliated Tongji Hospital and the Institute of Medical Genetics Affiliated to Tongji University
Abstract:Objective:To explore the association of the NKX2-5 gene with congenital heart disease (CHD). Methods:A cohort of 130 unrelated subjects with CHD and a total of 100 unrelated healthy individuals as controls were registered. The clinical data were recorded and the peripheral venous blood specimens were prepared. The complete exons and flanking partial introns of the candidate gene NKX2-5 were amplified by polymerase chain reaction and the amplicons were sequenced using the di-deoxynucleotide chain termination...
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