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胰岛素依赖型糖尿病的HLA基因型研究:DR3/DR4杂合子过多使得隐性假说不成立。

HLA genotypic study of insulin-dependent diabetes the excess of DR3/DR4 heterozygotes allows rejection of the recessive hypothesis.

作者信息

Rotter J I, Anderson C E, Rubin R, Congleton J E, Terasaki P I, Rimoin D L

出版信息

Diabetes. 1983 Feb;32(2):169-74. doi: 10.2337/diab.32.2.169.

DOI:10.2337/diab.32.2.169
PMID:6402405
Abstract

The genetics of insulin-dependent diabetes mellitus (IDDM) is currently an area of controversy, with some investigators proposing heterogeneity within the HLA region and even the existence of non-HLA-linked susceptibility genes, and others maintaining that a simple autosomal recessive gene linked to HLA with reduced penetrance is an adequate explanation. To resolve this latter question, we report here a simple method of testing whether a single HLA-linked susceptibility gene is inherited in a recessive fashion when it is associated with two different HLA alleles, as is the case for IDDM. It is shown that if the number of DR3/DR4 heterozygotes in a diabetic population exceeds the combined sum of DR3/3 and DR4/4 homozygotes in that same diabetic population, then a recessive mode of inheritance can be rejected. The advantages of the method are that it does not depend on ratios, as do relative risk calculations, nor does it depend on control data, but is based only on studies of the diabetics themselves. With data on 193 genotyped IDDM patients, we can clearly reject the recessive mode of inheritance, since the number of heterozygotes is 68 compared with a maximum of 22 homozygotes (P less than 10(-4)). Eight other published studies are in concordance with these results. Therefore, a nonparametric test, independent of the significance of any individual study, rejects equality of heterozygotes and homozygotes (P less than 0.002) and rejects the simple recessive mode of inheritance as a direct consequence. We conclude that more complex modes of inheritance of HLA-linked IDDM susceptibility, such as two different diabetogenic alleles or multiple loci, must be entertained. DIABETES 32:169-174, February 1983.

摘要

胰岛素依赖型糖尿病(IDDM)的遗传学目前是一个存在争议的领域,一些研究人员提出HLA区域内存在异质性,甚至存在与HLA无关的易感基因,而另一些人则坚持认为,与HLA连锁且外显率降低的简单常染色体隐性基因就足以解释。为了解决后一个问题,我们在此报告一种简单的方法,用于测试当单个与HLA连锁的易感基因与两种不同的HLA等位基因相关时(如IDDM的情况),它是否以隐性方式遗传。结果表明,如果糖尿病群体中DR3/DR4杂合子的数量超过该糖尿病群体中DR3/3和DR4/4纯合子数量之和,那么隐性遗传模式就可以被否定。该方法的优点在于,它不像相对风险计算那样依赖于比例,也不依赖于对照数据,而仅基于对糖尿病患者自身的研究。根据193名基因分型的IDDM患者的数据,我们可以明确否定隐性遗传模式,因为杂合子数量为68,而纯合子最多为22(P小于10^(-4))。其他八项已发表的研究与这些结果一致。因此,一种独立于任何单个研究显著性的非参数检验否定了杂合子和纯合子的相等性(P小于0.002),并直接否定了简单的隐性遗传模式。我们得出结论,必须考虑HLA连锁的IDDM易感性更复杂的遗传模式,例如两种不同的致糖尿病等位基因或多个基因座。《糖尿病》1983年2月第32卷:169 - 174页

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