胰岛素基因串联重复序列的可变数目决定成人隐匿性自身免疫性糖尿病的易感性。

Variable number of tandem repeats of the insulin gene determines susceptibility to latent autoimmune diabetes in adults.

作者信息

Cerrone Gloria Edith, Caputo Mariela, Lopez Ariel Pablo, González Claudio, Massa Carmen, Cédola Norberto, Targovnik Héctor Manuel, Frechtel Gustavo Daniel

机构信息

Laboratory of Molecular Biology, Department of Genetic and Molecular Biology, School of Pharmacy and Biochemistry, University of Buenos Aires, Buenos Aires, Argentina.

出版信息

Mol Diagn. 2004;8(1):43-9. doi: 10.1007/BF03260046.

DOI:10.1007/BF03260046

PMID:15230641

Abstract

BACKGROUND

The different clinical presentations of latent autoimmune diabetes in adults (LADA) and type 1 diabetes mellitus may be the result of susceptibility genes in determining the mode of onset. We analyzed the 5' polymorphisms of the insulin mini-satellite region (INS), a variable number of tandem repeats (VNTR) [repeat units; RU]. We evaluated the association of the different INS-VNTR alleles in patient susceptibility to LADA autoimmune diabetes. To our knowledge, this constitutes the first study of this kind performed in a Caucasian population.

METHODS

From an group of 160 Argentinean patients previously characterized as having LADA, we selected 44 patients who presented with humoral autoimmunity for genotyping and compared them to 88 patients with type 1 diabetes and 138 healthy individuals. The INS-VNTR allele classes were determined by Southern blotting (class I: 21-44RU; class III: 138-159RU). Subjects with class I alleles were further studied using PCR amplification to determine the exact length of the alleles (short 1S: 22-37RU; medium 1M: 38-41RU; large 1L: 42-43RU). Allelic and genotype frequencies were estimated by chi(2) tests for independence with 2 x 2 contingency tables and the relative risks (RR) were determined using GraphPad InStat software.

RESULTS

We observed differential associations among the class I alleles when comparing patients with LADA (80.6%) and type 1 diabetes (81.3%) with the controls (70%; p < 0.005). This increase was largely due to the high frequency of the 1S/S genotype (63.6% LADA vs 37% controls, with a p-value of 0.0019 [p1]; 53.4% type 1 diabetes vs 37% controls, with a p-value of 0.0149 [p2]). Remarkably, all LADA patients genotyped as class I homozygous had the shorter (S) class I allele (100%). Differences in the overall 1S distribution were observed: in LADA the 94.4% of the alleles were equal to or smaller than 35RU, while in patients with type 1 diabetes it was 78.3% and in controls 74.1%. Moreover, the relative risks associated with the 1S/S genotype for patients with LADA showed a substantial increase with respect to those with type 1 diabetes (52%) when we compare them to the controls (1S/S LADA/control, 2.282 [RR1] vs type 1 diabetes/control, 1.497 [RR2]).

CONCLUSION

The presence of the 1S allele could be considered a risk factor in LADA patients, as previously reported for type 1 diabetes. The class I INS-VNTR allele in LADA increases genetic susceptibility to disease development.

摘要

背景

成人隐匿性自身免疫性糖尿病（LADA）和1型糖尿病的不同临床表现可能是由易感基因决定发病方式所致。我们分析了胰岛素微卫星区域（INS）5'端的多态性，即可变数目串联重复序列（VNTR）[重复单位；RU]。我们评估了不同的INS - VNTR等位基因与LADA自身免疫性糖尿病患者易感性之间的关联。据我们所知，这是在白种人群中进行的此类首次研究。

方法

从一组先前被诊断为LADA的160名阿根廷患者中，我们选取了44名出现体液自身免疫的患者进行基因分型，并将他们与88名1型糖尿病患者和138名健康个体进行比较。通过Southern印迹法确定INS - VNTR等位基因类别（I类：21 - 44RU；III类：138 - 159RU）。对具有I类等位基因的受试者进一步使用PCR扩增来确定等位基因的确切长度（短1S：22 - 37RU；中1M：38 - 41RU；长1L：42 - 43RU）。通过卡方检验独立性对2×2列联表估计等位基因和基因型频率，并使用GraphPad InStat软件确定相对风险（RR）。

结果

在将LADA患者（80.6%）和1型糖尿病患者（81.3%）与对照组（70%）进行比较时，我们观察到I类等位基因之间存在差异关联（p < 0.005）。这种增加主要归因于1S/S基因型的高频率（LADA患者中为63.6%，对照组为37%，p值为0.0019 [p1]；1型糖尿病患者中为53.4%，对照组为37%，p值为0.0149 [p2]）。值得注意的是，所有基因分型为I类纯合子的LADA患者都具有较短的（S）I类等位基因（100%）。观察到1S总体分布存在差异：在LADA患者中，94.4%的等位基因等于或小于35RU，而在1型糖尿病患者中为78.3%，在对照组中为74.1%。此外，当我们将LADA患者与对照组相比时，与1S/S基因型相关的相对风险相对于1型糖尿病患者有显著增加（52%）（1S/S LADA/对照组，2.282 [RR1] 对比1型糖尿病/对照组，1.497 [RR2]）。