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以色列犹太人的类风湿性关节炎:DRB1等位基因第三高变区的共享序列与易感性相关。

Rheumatoid arthritis in Israeli Jews: shared sequences in the third hypervariable region of DRB1 alleles are associated with susceptibility.

作者信息

Gao X, Gazit E, Livneh A, Stastny P

机构信息

Department of Internal Medicine, University of Texas, Southwestern Medical Center, Dallas 75235-8886.

出版信息

J Rheumatol. 1991 Jun;18(6):801-3.

PMID:1895259
Abstract

Rheumatoid arthritis (RA) is known to be associated with class II HLA antigens in most populations, but recent studies in Israeli Jewish patients showed no significant differences in either DR4 or DR1 between patients and controls. In a previous DR4 subset study we found DR4-Dw15 to be associated with susceptibility (RR = 9.2) but this allele occurred in only 12% of the patients. We analyzed all DRB1 genes, using the polymerase chain reaction (PCR) and hybridization with allele specific oligonucleotides, in 49 Jewish patients with RA and 40 normal Jewish controls. Six DRB1 alleles that are similar to the prototype DR4-Dw4 (DRB10401) appeared to contribute to the risk for developing RA. In addition to DR4-Dw15 (DRB10405) 2 other alleles having substitutions in codons 71 only (DR1-Dw1/DRB10101, DR4-Dw14.2/DRB10408) or in codons 70 and 71 (DRw10/DRB11001) gave highly significant relative risks. Together, this group, with valine in position 85, and glycine in codon 86, gave a relative risk of 11.0 (p = 0.0002). Two other alleles with the same sequence in the third hypervariable region (amino acids 67-74) but with valine in codon 86 (DR4-Dw14.1/DRB10404) or alanine in 85 and valine in 86 (DR1-Dw20, DRB1*0102) gave a combined risk of 3.6 (p = 0.049). Altogether these 7 alleles with similar sequences in the third hypervariable region accounted for 55.6% of the patients, with an overall relative risk of 8.6 (p = 0.00002). Our results in this population indicate that shared epitopes in the third hypervariable region of DRB1 alleles also play a role in susceptibility to RA.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在大多数人群中,类风湿性关节炎(RA)与II类HLA抗原相关,但最近对以色列犹太患者的研究表明,患者与对照组在DR4或DR1方面均无显著差异。在之前一项针对DR4亚组的研究中,我们发现DR4-Dw15与易感性相关(相对危险度RR = 9.2),但该等位基因仅出现在12%的患者中。我们使用聚合酶链反应(PCR)及等位基因特异性寡核苷酸杂交技术,对49例患RA的犹太患者和40名正常犹太对照者的所有DRB1基因进行了分析。六个与原型DR4-Dw4(DRB10401)相似的DRB1等位基因似乎与患RA的风险有关。除了DR4-Dw15(DRB10405)外,另外两个仅在密码子71有替换的等位基因(DR1-Dw1/DRB10101、DR4-Dw14.2/DRB10408)或在密码子70和71有替换的等位基因(DRw10/DRB11001)具有高度显著的相对危险度。这一组在第85位为缬氨酸、第86位为甘氨酸,其相对危险度为11.0(p = 0.0002)。另外两个在第三高变区(氨基酸67 - 74)具有相同序列,但第86位为缬氨酸的等位基因(DR4-Dw14.1/DRB10404)或第85位为丙氨酸、第86位为缬氨酸的等位基因(DR1-Dw20,DRB1*0102)的合并危险度为3.6(p = 0.049)。在第三高变区具有相似序列的这7个等位基因总共占患者的55.6%,总体相对危险度为8.6(p = 0.00002)。我们在这一人群中的研究结果表明,DRB1等位基因第三高变区的共享表位在RA易感性中也起作用。(摘要截选至250词)

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