首页> 外文期刊>Diabetes >'Extended' A1, B8, DR3 Haplotype Shows Remarkable Linkage Disequilibrium but Is Similar to Nonextended Haplotypes in Terms of Diabetes Risk.
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'Extended' A1, B8, DR3 Haplotype Shows Remarkable Linkage Disequilibrium but Is Similar to Nonextended Haplotypes in Terms of Diabetes Risk.

机译:“扩展的” A1,B8,DR3单倍型显示出显着的连锁不平衡,但就糖尿病风险而言,与非扩展的单倍型相似。

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To evaluate potential differential diabetes risk of DR3 haplotypes we have evaluated class I alleles as well as two microsatellites previously associated with differential risk associated with DR3 haplotypes. We found that over one-third of patient DR3 chromosomes consisted of an extended DR3 haplotype, from DQ2 to D6S2223 (DQ2, DR3, D6S273-143, MIC-A5.1, HLA-B8, HLA-Cw7, HLA-A1, and D6S2223-177) with an identical extended haplotype in controls. The extended haplotype was present more frequently (35.1% of autoimmune-associated DR3 haplotypes, 39.4% of control DR3 haplotypes) than other haplotypes (no other haplotype >5% of DR3 haplotypes) and remarkably conserved, but it was not transmitted from parents to affected children more frequently than nonconserved DR3-bearing haplotypes. This suggests that if all alleles are truly identical for the major A1, B8, DR3 haplotype (between A1 and DR3), with different alleles on nonconserved haplotypes without differential diabetes risk, then in this region of the genome DR3-DQ2 may be the primary polymorphisms of common haplotypes contributing to diabetes risk.
机译:为了评估DR3单倍型的潜在差异性糖尿病风险,我们评估了I类等位基因以及两个以前与DR3单倍型相关的差异风险相关的微卫星。我们发现,超过三分之一的患者DR3染色体由扩展的DR3单倍型组成,从DQ2到D6S2223(DQ2,DR3,D6S273-143,MIC-A5.1,HLA-B8,HLA-Cw7,HLA-A1和D6S2223-177),且在对照中具有相同的扩展单倍型。延伸单倍型比其他单倍型(其他单倍型> DR3单倍型的5%)更频繁地出现(自身免疫相关DR3单倍型的35.1%,对照DR3单倍型的39.4%),并且显着保守,但是它没有从父母传播给受感染的儿童比不保守的携带DR3的单倍型患病的频率更高。这表明,如果主要A1,B8,DR3单倍型(在A1和DR3之间)的所有等位基因真正相同,非保守单倍型上的等位基因不同,且没有糖尿病风险,那么在该基因组区域中,DR3-DQ2可能是主要的常见单倍型的多态性导致糖尿病风险。

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