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荷兰胰岛素依赖型糖尿病中的HLA和GM:一项综合多重家庭与人群研究报告

HLA and GM in insulin-dependent diabetes in the Netherlands: report on a combined multiplex family and population study.

作者信息

de Jongh B M, Bruining G J, Schreuder G M, Schuurman R K, Radder J K, van Loghem E, Meera Khan P, Hauptmann G, van Rood J J

出版信息

Hum Immunol. 1984 May;10(1):5-21. doi: 10.1016/0198-8859(84)90082-x.

Abstract

This report deals with the genetic factors involved in insulin-dependent diabetes mellitus (IDD) in The Netherlands. Twenty-two Dutch multiplex families with IDD were typed for HLA-A, -B, -C, and -DR antigens, for BF, C2, C4, and GLO polymorphisms, as well as for GM allotypes of immunoglobulins. In addition, 53 unrelated IDD children and 31 unrelated patients with adult onset IDD were typed for HLA-A, -B, -C, and -DR antigens. A significant heterogeneity for the frequency of HLA-DR4 related to age of onset was observed. A significant deviation of the Hardy-Weinberg equilibrium was observed for the HLA-DR locus with an excess in patients of heterozygotes HLA-DR3, -DR4.HLA-B8, and HLA-B15 were not only secondary associated, but constituted with HLA-DR3 and -DR4, respectively, a haplotype in association with IDD. Nonrandom segregation of HLA-haplotypes was observed in multiplex families exemplified by an excess of HLA-identical affected sibpairs . Cross- overs between HLA-DR and GLO identified the HLA-DR segment as mainly involved in the association with IDD. Three diabetic haplotypes were confirmed to occur frequently among affected sibs: (a) A1, B8, BFS, C2.1, C4AQO , C4B1 ,DR3, GLO2 ; (b) Aw30, Cw5 ,B18,BFF1,C2.1, C4A3 , C4BQO ,DR3, GLO2 ; (c) A2,Cw3, B15,BFS, C2.1, C4A3 , C4B3 , DR4,GLO1. The segregation of GM allotypes to affected sibpairs was not significantly different from random segregation. The main conclusions from this study are that significant heterogeneity for age of onset exists and that the data are not compatible with simple genetic models including dominant, recessive, and intermediate models of inheritance. The data do require more complex models, involving two different HLA-linked (sets of) susceptibility genes.

摘要

本报告探讨了荷兰胰岛素依赖型糖尿病(IDD)所涉及的遗传因素。对22个患有IDD的荷兰多重家庭进行了HLA - A、- B、- C和 - DR抗原分型,以及BF、C2、C4和GLO多态性分型,还有免疫球蛋白的GM同种异型分型。此外,对53名无亲缘关系的IDD儿童和31名无亲缘关系的成年发病IDD患者进行了HLA - A、- B、- C和 - DR抗原分型。观察到与发病年龄相关的HLA - DR4频率存在显著异质性。在HLA - DR位点观察到显著偏离哈迪 - 温伯格平衡,患者中杂合子HLA - DR3、- DR4、HLA - B8和HLA - B15过多。HLA - B8和HLA - B15不仅是次要关联,而且分别与HLA - DR3和 - DR4构成与IDD相关的单倍型。在多重家庭中观察到HLA单倍型的非随机分离,以HLA相同的患病同胞对过多为例。HLA - DR和GLO之间的交叉确定HLA - DR区段主要与IDD关联有关。确认三种糖尿病单倍型在患病同胞中频繁出现:(a)A1、B8、BFS、C2.1、C4AQO、C4B1、DR3、GLO2;(b)Aw30、Cw5、B18、BFF1、C2.1、C4A3、C4BQO、DR3、GLO2;(c)A2、Cw3、B15、BFS、C2.1、C4A3、C4B3、DR4、GLO1。GM同种异型向患病同胞对的分离与随机分离无显著差异。本研究的主要结论是发病年龄存在显著异质性,并且数据与包括显性、隐性和中间遗传模型在内的简单遗传模型不相符。数据确实需要更复杂的模型,涉及两个不同的与HLA连锁的(一组)易感基因。

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