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部分基因组扫描研究2型糖尿病易感基因座位的初步报告
引用本文:骆天红,赵萸,袁文涛,李果,黄薇,王琴琴,郁忠勤,赵家军,何海屏,杨明功,孙卫华,戴蒙,江凌,左祥生,陈家伦,罗敏. 部分基因组扫描研究2型糖尿病易感基因座位的初步报告[J]. 中华内分泌代谢杂志, 2000, 16(3): 160-163
作者姓名:骆天红  赵萸  袁文涛  李果  黄薇  王琴琴  郁忠勤  赵家军  何海屏  杨明功  孙卫华  戴蒙  江凌  左祥生  陈家伦  罗敏
作者单位:1. 200025,上海第二医科大学附属瑞金医院,上海市内分泌研究所
2. 200025,上海第二医科大学附属瑞金医院,分子医学中心
3. 200025,上海第二医科大学附属瑞金医院,国家人类基因组南方研究中心
4. 山东省立医院
5. 上海市静安区中心医院
基金项目:国家科委 863重大基础科研基金!(2 19 0 1 0 2 0 2,973重大基础科研基金!资助项目G19980 5 0 0 2 )
摘    要:目的 通过部分基因组扫描筛查与 2型糖尿病连锁的位点 ,为进一步定位和克隆 2型糖尿病的易感基因奠定基础。方法 采用以微卫星DNA标记为基础的荧光标记 半自动基因组扫描技术 ,应用Perkin Elmer的试剂盒 (ABIPrismLinkageMappingSetVersion 2 ) ,共 6 3对引物 ,研究 2型糖尿病家系 5 8个 ,共 2 6 4份样品 ,其中糖尿病患者 15 2人 ,非糖尿病患者 112人 ,有同胞关系的患者74人 ,组成 45对患病同胞对 ,对 1号、12号、18号、2 0号染色体进行部分基因组扫描。连锁分析采用GENEHUNTERversion 2连锁分析软件包。结果 非参数连锁分析结果提示 ,1号染色体 1p31区域的D1S2 86 8位点同 2型糖尿病连锁 ,其NPL值为 1.192 ,P值为 0 .0 45 ,2 0号染色体短臂末端 2 0 p13区域的位点D2 0S117和D2 0S889以及 2 0号染色体长臂 2 0q13 .3区域的D2 0S196位点同 2型糖尿病连锁 ,其NPL值分别为 1.36 2、1.36 0、1.199,P值分别为 0 .0 30、0 .0 30和 0 .0 49。结论  1号染色体短臂 1p31区域及 2 0号染色体短臂 2 0 p13区域及长臂 2 0 q13.3区域可能存在有 2型糖尿病的易感基因。

关 键 词:糖尿病  非胰岛素依赖型  微随体重复(微卫星标记)  人基因组项目  连锁分析

A genome scan for late onset type 2 diabetes susceptibility loci in Chinese: a preliminary report
LUO Tianhong ,ZHAO Yu,YUAN Wentao,et al.. A genome scan for late onset type 2 diabetes susceptibility loci in Chinese: a preliminary report[J]. Chinese Journal of Endocrinology and Metabolism, 2000, 16(3): 160-163
Authors:LUO Tianhong   ZHAO Yu  YUAN Wentao  et al.
Affiliation:LUO Tianhong *,ZHAO Yu,YUAN Wentao,et al. *Shanghai Institute of Endocrinology,Reijin Hospital,Shanghai Second Medical University,Shanghai 200025
Abstract:Objective To identify loci influencing susceptibility to late onset type 2 diabetes mellitus by genome scan method. Methods Genome scan method based on fluorescence labeled microsatellite markers with multiplex PCR system was used to identify loci influencing susceptibility to late onset type 2 diabetes mellitus. The 63 pairs of primers of microsatellits DNA markers used in this study were provided by Perkin Elmer Applied Biosystems Division. 264 samples from 58 pedigrees were studied. Among these samples, 152 were collected from diabetic patients including 74 affected siblings forming 45 affected sib pairs and 112 from non diabetic members. Chromosome 1, 12, 18, 20 were scanned and linkage analysis were carried out with GENEHUNTER (version 2) software. Results Non parametric linkage analysis showed evidence for linkage at several chromosome regions with type 2 diabetes mellitus, including D1S2868 at 1p31, with NPL value of 1.192 and p value of 0.045, and D20S177, D20S889, D20S196 at 20p13, 20p13 and 20q13.3 respectively, withNPL valueof1.362,1.360,and 1.199 respectively and p value of 0.030, 0.030 and 0.049 respectively. Conclusion Loci on region 1p31, 20p13 and 20q13.3 may influence susceptibility to type 2 diabetes.
Keywords:Diabetes mellitus   non insulin dependent  Microsatellite repeats  Human genome project  Linkage analysis
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