Margaritte-Jeannin P, Clerget-Darpoux F, Hors J, Deschamps I
Unité de Recherches de Génétique Epidémiologique (INSERM U155), Paris, France.
Am J Hum Genet. 1995 May;56(5):1080-7.
Among patients with insulin-dependent diabetes mellitus (IDDM), an excess of DR3 and DR4 alleles is classically described when compared with the general population. In addition, an excess of maternal DR3 and paternal DR4 alleles among patients (DR3DR4) is observed. In order to explain these observations, two alternative hypotheses can be tested: maternal effect and parental imprinting. Maternal effect has been tested and not rejected on a sample of 416 caucasians affected with IDDM. Under this hypothesis, the children of a DR3 mother are expected to have an earlier exposure and, hence, an earlier age at onset. However, we did not observe such a difference in age at onset in this data set. Using the marker-association-segregation-chi 2 method, we have tested four hypotheses with different parental effects of two susceptibility alleles, alpha 0 and beta 0, at two different closely linked loci. Under the hypothesis that best fitted the data, the probability of being affected depended on the parental inheritance of the susceptibility alleles, suggesting parental imprinting (i.e., differential role of maternal and paternal allele), without evidence for a cis-trans effect. We conclude that parental imprinting on a specific allelic combination may explain the observations on the HLA genotypes of the patients and their relatives.
在胰岛素依赖型糖尿病(IDDM)患者中,与普通人群相比,经典描述为DR3和DR4等位基因过量。此外,还观察到患者中母亲的DR3和父亲的DR4等位基因过量(DR3DR4)。为了解释这些观察结果,可以检验两种替代假说:母体效应和父母印记。在416名受IDDM影响的白种人样本中,已经检验了母体效应且未被否定。在这个假说下,预计DR3母亲的孩子会有更早的暴露,因此发病年龄更早。然而,在这个数据集中我们没有观察到发病年龄的这种差异。使用标记-关联-分离-卡方检验方法,我们在两个不同紧密连锁的位点上,检验了关于两个易感等位基因α0和β0的不同亲本效应的四个假说。在最符合数据的假说下,受影响的概率取决于易感等位基因的亲本遗传,提示父母印记(即母源和父源等位基因的不同作用),但没有顺式-反式效应的证据。我们得出结论,对特定等位基因组合的父母印记可能解释了对患者及其亲属HLA基因型的观察结果。
