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留尼汪岛1型糖尿病家族中HLA单倍型分析

Analysis of HLA haplotypes in families with type 1 diabetes mellitus in La Réunion island.

作者信息

Feugeas J P, Tortosa P, Dulay S, Augustin-Pascalis I, Charron D, Krishnamoorthy R, Caillens H, Montchamp-Moreau C

机构信息

Laboratoire d'Immunologie et d'Histocompatibilité, Hôpital Saint-Louis, Paris, France.

出版信息

Eur J Immunogenet. 1996 Dec;23(6):459-70. doi: 10.1111/j.1744-313x.1996.tb00136.x.

Abstract

To analyse HLA and insulin-dependent diabetes mellitus (IDDM) association in the ethnically mixed population of La Réunion island, we carried out a family study on 70 diabetic subjects. HLA-DQA1, -DQB1 and -DRB1 typing was performed by polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP), completed by PCR-sequence-specific oligonucleotide (SSO) and PCR-sequence-specific priming (SSP). Haplotype-relative risks (HRR) were determined with the non-transmitted parental haplotypes as controls, and relative risks (RR) were calculated with a classical case-control study. The most significant risks were found for the cis and trans combinations between DQA103 or 0501 (Arg52+) and DQB102 or 0302 (Asp57-) alleles, suggesting a direct role for the HLA-DQ heterodimer in IDDM susceptibility. Interestingly, due to the mixed origin of the population, the trans-encoded DQ molecules in the (DR3)-DQA10501-DQB102/(DR4)-DQA103-DQB10302 subjects were also found cis-encoded in patients with the (DR7 or 9)-DQA103-DQB102 haplotype and in a patient with the rare (DR11)-DQA10501-DQB10302 haplotype. A relative predispositional effect (RPE) analysis gave significant haplotype-IDDM+ associations in the following order: (DR3)-DQA10501-DQB102 > (DR4)-DQA103-DQB10302 > (DR9)-DQA103- DQB02 > (DR7)-DQA103-DQB102 > (DR2)-DQA101-DQB10502. No protective effect remained significant once the susceptible haplotypes were removed. A stratification study showed a stronger influence of the DQ genes than DRB1 alleles within the DR7 haplotypes. On the other hand, IDDM subjects with only one susceptible haplotype had inherited this haplotype more often from their father than from their mother. This paternal effect could be related to the greater risk of IDDM in offspring of diabetic fathers than the risk in offspring of diabetic mothers.

摘要

为分析留尼汪岛多民族混合人群中HLA与胰岛素依赖型糖尿病(IDDM)的关联,我们对70名糖尿病患者进行了家系研究。通过聚合酶链反应-限制性片段长度多态性(PCR-RFLP)对HLA-DQA1、-DQB1和-DRB1进行分型,并通过PCR-序列特异性寡核苷酸(SSO)和PCR-序列特异性引物(SSP)加以完善。以未传递的亲代单倍型作为对照确定单倍型相对风险(HRR),并通过经典病例对照研究计算相对风险(RR)。发现DQA103或0501(Arg52+)与DQB102或0302(Asp57-)等位基因之间的顺式和反式组合风险最为显著,提示HLA-DQ异二聚体在IDDM易感性中起直接作用。有趣的是,由于人群来源混合,在(DR3)-DQA10501-DQB102/(DR4)-DQA103-DQB10302受试者中反式编码的DQ分子,在具有(DR7或9)-DQA103-DQB102单倍型的患者以及具有罕见的(DR11)-DQA10501-DQB10302单倍型的一名患者中也为顺式编码。相对易感性效应(RPE)分析得出单倍型与IDDM+之间存在显著关联,顺序如下:(DR3)-DQA10501-DQB102 > (DR4)-DQA103-DQB10302 > (DR9)-DQA103-DQB02 > (DR7)-DQA103-DQB102 > (DR2)-DQA101-DQB10502。去除易感单倍型后,未发现有显著的保护作用。分层研究显示,在DR7单倍型中,DQ基因的影响比DRB1等位基因更强。另一方面,仅携带一种易感单倍型的IDDM患者从父亲那里遗传该单倍型的频率高于从母亲那里遗传的频率。这种父系效应可能与糖尿病父亲的后代患IDDM的风险高于糖尿病母亲的后代有关。

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