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胰岛素受体底物-4基因多态性与2型糖尿病的相关性研究 被引量:1

Association study of insulin receptor substrate-4 gene polymorphism with type 2 diabetes
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摘要 目的 研究北京地区汉族人群胰岛素受体底物 4 (IRS 4 )基因密码子 879c g多态性与 2型糖尿病的相关性。 方法 采用配偶对作病例 对照研究。用聚合酶链反应 (PCR) 限制性内切酶片段长度多态性 (RFLP)的方法检测IRS 4基因密码子 879c g多态性。 结果  ( 1)男性与女性间IRS 4基因密码子 879c g多态性分布特点不同 ,男性无杂合子。g等位基因频率为男性 6 1.8%,女性6 3 .9%。 ( 2 )此多态性位点的基因型频率和等位基因频率在 2型糖尿病组和对照组间差异无显著意义。 ( 3)在男性对照组中 ,可见gg基因型组胰岛 β细胞功能指数低于cc基因型组。  结论 北京地区汉族人群中IRS 4基因密码子 879c g多态性与 2型糖尿病无明显相关性。 Objective To study the association of insulin receptor substrate-4 (IRS-4) gene codon 879 c/g polymorphism with type 2 diabetes and its intermediate phenotypes in Chinese population in Beijing. Methods The IRS-4 gene codon 879 c/g polymorphism was detected by polymerase chain reaction and appropriate restriction enzyme (PCR-RFLP) in 110 type 2 diabetic cases and 80 normal controls. Results (1) There was different genotype distribution of IRS-4 codon 879 c/g polymorphism between the male and female groups. No heterozygote was found in male. The frequence of allele g was 61.8% in male and 63.9% in female respectively. (2) The genotype frequency and allelic frequency of the polymorphism were not significantly different between diabetics and control groups. (3) The islet β cell function index was lower in the individuals carrying the gg genotype than those carrying the cc genotype in male control group. Conclusions The gg geneotype of human IRS-4 codon 879 c/g polymorphism alone has no association with type 2 diabetes in northern Chinese population.
作者 王海宁 洪天配 徐希平
机构地区 北京大学第三医院内分泌科 北京大学生态遗传与生殖卫生研究中心
出处 《中国糖尿病杂志》 CAS CSCD 2003年第3期188-191,共4页 Chinese Journal of Diabetes
基金 教育部留学回国人员启动资金 中华医学基金专项人才基金资助项目
关键词 胰岛素受体底物-4 基因多态性 2型糖尿病 IRS-4 血糖 Type 2 diabetes mellitus Insulin Gene Polymorphism
分类号 R587.1 [医药卫生—内分泌]
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参考文献10

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同被引文献15

  • 1黄青阳,彭姝彬,杜纪坤,程孟荣,姬森林.2型糖尿病候选基因的研究进展[J].国际遗传学杂志,2006,29(6):446-453. 被引量:8
  • 2王延庆,项坤三,郑泰山,贾伟平,沈坤雪,李杰.NIDDM1位点钙蛋白酶-10基因UCSNP44的变异及其对2型糖尿病患者血糖的影响[J].中华医学杂志,2002,82(9):613-616. 被引量:4
  • 3姬森林,黄青阳.PPARγ变异与复杂疾病[J].遗传,2006,28(8):993-1001. 被引量:4
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  • 5Altshuler D, Hirschhorn JN, Klannemark M, et al. The common Pl?ARgamma Prol2Ala polymorphism is associated with decreased risk of type 2 diabetes[J]. Nat Genet, 2000,26( 1 ) : 76-80.
  • 6Love-Gregol7 L, Wasson J, Lin J, et al. E23K single nueleotide polymorphisnl in the islet ATP-sensitive potassium channel gene (Kit6.2) contributes as much to the risk of Type Ⅱ diabetes in Caucasians as the PPARgamma Pro l2Ala variant [J ]. Diabetologia, 2003,46( 1 ) : 136-137.
  • 7Horikawa Y, Oda N, Cox N J, et al. Genetic variation in the gene encoding calpain-lO is associated with type 2 diabetes mellitus [ J ]. Nat Genet, 2000,26 (2) : 163-175.
  • 8Uchida T, Myers MG Jr, White MF. IRS-4 mediates protein kinase B signaling during insulin stimulation without promoting antiapoptosis[J]. Mol Cell Biol,2000,20(1) : 126-138.
  • 9Almind K, Frederiksen SK, Ahlgren MG, et al. Common amino acid substitutions in insulin receptor substrate-4 are not associated with Type Ⅱ diabetes mellitus or insulin resistance[J]. Diabetologia, 1998,41 ( 8 ) : 969-974.
  • 10Veiga-da-Cunha M, Van Schaftingen E. Identification of fructose 6-phosphate- and fructose 1-phosphate-binding residues in the regulatory protein of glucokinase[ J]. J Biol Chem, 2002,277 (10) :8466-8473.

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中国糖尿病杂志
2003年 第3期

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