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中国人早发性糖尿病GCK基因突变的筛查 被引量:3

Mutation screening of GCK gene in Chinese early-onset diabetes population
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摘要 目的了解葡萄糖激酶(glucokinase)基因GCK突变和序列变异在中国人早发性糖尿病人群中的发生情况。方法应用直接测序方法对174名无亲缘关系中国人(其中80名为非糖尿病对照组,94例为早发性糖尿病家系先证者)进行GCK基因启动子区、10个外显子及其侧翼内含子区筛查。结果未在编码区发现突变,但发现几种先前已经报道的序列变异外显子1a的5′非翻译区,位于翻译起始点上游84bp处GGCGG→GGGGG(糖尿病组G等位基因频率0·106比对照组0.075,P=0.355);IVS1b+12(A→T)(糖尿病组T等位基因频率0·005而在对照组未发现该变异);IVS5+29(G→T)(糖尿病组T等位基因频率0.027比对照组0.019,P=0·731);IVS9+8(T→C)(糖尿病组C等位基因频率0.585比对照组0.694,P=0.044)。此外,还发现1个未被报道的新的序列变异IVS9+49(G→A)(糖尿病组A等位基因频率0.011比对照组0.006,P=1.000)。未发现外显子1a的5′非翻译区,-84bp处(C→G)、IVS5+29(G→T)、IVS9+8(T→C)和IVS9+49(G→A)变异与血糖、胰岛素、C-肽及空腹血脂谱等临床变量相关。结论GCK基因突变不是中国人早发性糖尿病发病的主要原因。 Objective To investigate the prevalence of mutations and sequence variations of glucokinase gene GCK in Chinese early-onset diabetes population. Methods The study was conducted in 174 unrelated Chinese residents, including 80 nondiabetic controls, 94 probands of early-onset diabetes pedigree. Direct sequencing was performed to screen all 10 exons of glucokinase gene, including promoter and exon/intron junctions. Results No mutations were identified in coding region, but several previously reported sequence variants were identified. 5'-untranslated region of exon la, 84 bp upstream of the translation initiation site GGCGG→GGGGG(early-onset diabetes group G allele frequency 0.106 vs control group 0.075, P = 0.355) ; IVS1b + 12 (A→T) (early-onset diabetes group T allele frequency 0.005 vs non-identity of this variation in control group) ; IVS 5 + 29 (G→T) (early-onset diabetes group T allele frequency 0. 027 v s control group 0.019, P = 0. 731 ); IVS 9 + 8 (T→ C) (early-onset diabetes group C allele frequency 0. 585 vs 0.694, P =0.044). A novel variation IVS 9 + 49 (G→A) (early-onset diabetes group A allele frequency 0.011 vs control 0.006, P = 1.000) was identified. There were no significant relationships of the exon la 5'-UTR - 84 bp(C→ G) ,IVS 5 + 29 (G→T) ,IVS 9 + 8 (T→C) and IVS 9 + 49 (G→A) variants of GCK gone to the clinical variables such as plasma glucose, insulin, C-peptide and fasting lipid profile. Conclusion The prevalence of structural mutations in glucokinase gene responsible for early-onset diabetes appears to be rare among Chinese patients.
作者 郑泰山 吴松华 杨震 陆惠娟 项坤三
机构地区 上海交通大学附属第六人民医院内分泌代谢科
出处 《中华医学遗传学杂志》 CAS CSCD 北大核心 2005年第6期671-674,共4页 Chinese Journal of Medical Genetics
基金 国家自然科学基金(30470813) 上海市自然科学基金(01ZB14047)~~
关键词 早发性糖尿病 葡萄糖激酶基因 直接测序 early-onset diabetes glucokinase gene direct sequencing
分类号 R587.1 [医药卫生—内分泌] R734.2 [医药卫生—内科学]
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参考文献7

  • 1Fajans SS, Bell GI, Polonsky KS. Molecular mechanism and clinical pathophysiology of maturity-onset diabetes of the young. N Engl J Med, 2001,345: 971-980. 被引量:1
  • 2Gloyn AL. Glucokinase (GCK) mutations in hyper- and hypo-glycemia: maturity-onset diabetes of the young, permanent neonatal diabetes, and hyperinsulinemia of infancy. Hum Mutat, 2003,22: 353-362. 被引量:1
  • 3Froguel P, Zouali H, Vionnet N, et al. Familial hyperglycemia due to mutations in glucokinase, definition of a subtype of diabetes mellitus. N Engl JMed, 1993, 328: 697-702. 被引量:1
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中华医学遗传学杂志
2005年 第6期

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