Shaw J T, Lovelock P K, Kesting J B, Cardinal J, Duffy D, Wainwright B, Cameron D P
Department of Diabetes and Endocrinology, Princess Alexandra Hospital, Brisbane, Queensland, Australia.
Diabetes. 1998 Nov;47(11):1793-6. doi: 10.2337/diabetes.47.11.1793.
NIDDM has a substantial genetic component, but the nature of the genetic susceptibility is largely unknown. Maturity-onset diabetes of the young (MODY) is a genetically heterogeneous monogenic form of NIDDM characterized by an early age of onset and autosomal dominant inheritance, and linkage studies have identified genes that are mutated in different MODY pedigrees on chromosome 20 (MODY1 locus, hepatocyte nuclear factor-4alpha [HNF-4alpha] gene), chromosome 7 (MODY2 locus, glucokinase gene), and chromosome 12 (MODY3 locus, HNF-1alpha gene). We studied an extended pedigree in which multiple members are affected by late-onset NIDDM associated with insulin resistance and performed linkage analysis with four microsatellite markers in the MODY3 region of chromosome 12q. We found significant evidence for linkage between NIDDM and the MODY3 locus (logarithm of odds score 3.65 at theta = 0.008 telomeric to marker D12S321), but sequencing of the 10 exons and promoter of HNF-1alpha did not identify any causative mutation in this gene. Our results indicate that the region of chromosome 12q close to MODY3 harbors a novel susceptibility gene or genes for NIDDM.
非胰岛素依赖型糖尿病(NIDDM)具有很大的遗传成分,但遗传易感性的本质在很大程度上尚不清楚。青年发病的成年型糖尿病(MODY)是NIDDM的一种遗传异质性单基因形式,其特征为发病年龄早且呈常染色体显性遗传,连锁研究已确定在20号染色体(MODY1位点,肝细胞核因子-4α[HNF-4α]基因)、7号染色体(MODY2位点,葡萄糖激酶基因)和12号染色体(MODY3位点,HNF-1α基因)上不同MODY家系中发生突变的基因。我们研究了一个扩大的家系,其中多个成员患有与胰岛素抵抗相关的晚发性NIDDM,并使用位于12号染色体q臂MODY3区域的四个微卫星标记进行连锁分析。我们发现了NIDDM与MODY3位点之间存在连锁的显著证据(在距标记D12S321端粒方向θ = 0.008处,优势对数得分3.65),但对HNF-1α的10个外显子和启动子进行测序未发现该基因有任何致病突变。我们的结果表明,12号染色体q臂上靠近MODY3的区域含有一个或多个新的NIDDM易感基因。
