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人类白细胞抗原杂合性会增加患类风湿性关节炎的易感性。

HLA heterozygosity contributes to susceptibility to rheumatoid arthritis.

作者信息

Wordsworth P, Pile K D, Buckely J D, Lanchbury J S, Ollier B, Lathrop M, Bell J I

机构信息

Institute of Molecular Medicine, Oxford, England.

出版信息

Am J Hum Genet. 1992 Sep;51(3):585-91.

Abstract

We have investigated the role of HLA-DR genotypes in 184 patients with severe rheumatoid arthritis (RA) and in 46 patients with Felty syndrome, to establish the relative contribution of the RA-associated subtypes of DR4 (Dw4, Dw14, and Dw15). There was an excess of DR4 homozygotes, particularly Dw4/Dw14 compound heterozygotes (relative risk [RR] 49). The risk associated with Dw4 depended on the other allele present--Dw4/DR1 (RR 21), Dw4/Dw4 (RR 15), and Dw4/DRX (RR 6). There was a significant risk from Dw4/Dw14 compared with Dw4/Dw4, both in those with severe RA (RR 2.9; P less than .02) and in those with Felty syndrome (RR 4.2; P less than .02). In contrast, in a further 63 known DR4 homozygotes with RA, not selected for severe disease, the excess of Dw4/Dw14 was much less striking (RR 1.4; not significant), suggesting that this genotype may be particularly associated with more severe disease. We also found four cases with the rare Dw4/Dw15 genotype (expected less than or equal to 0.5; P less than or equal to .02). Since the Dw4, Dw14, Dw15, and DR1 molecules have similar antigen-binding sites and since combinations of these alleles particularly predispose to severe RA, we suggest that synergistic mechanisms are involved. These could include an effect on T-cell repertoire selection.

摘要

我们研究了HLA - DR基因型在184例严重类风湿关节炎(RA)患者和46例费尔蒂综合征患者中的作用,以确定与RA相关的DR4亚型(Dw4、Dw14和Dw15)的相对贡献。DR4纯合子过多,尤其是Dw4 / Dw14复合杂合子(相对风险[RR]为49)。与Dw4相关的风险取决于存在的另一个等位基因——Dw4 / DR1(RR为21)、Dw4 / Dw4(RR为15)和Dw4 / DRX(RR为6)。与Dw4 / Dw4相比,Dw4 / Dw14在严重RA患者(RR为2.9;P小于0.02)和费尔蒂综合征患者(RR为4.2;P小于0.02)中均有显著风险。相比之下,在另外63例已知的患有RA的DR4纯合子中(未因严重疾病而被选择),Dw4 / Dw14的过量情况则不那么明显(RR为1.4;无显著性),这表明该基因型可能与更严重的疾病特别相关。我们还发现了4例罕见的Dw4 / Dw15基因型病例(预期小于或等于0.5;P小于或等于0.02)。由于Dw4、Dw14、Dw15和DR1分子具有相似的抗原结合位点,且这些等位基因的组合特别易患严重RA,我们认为涉及协同机制。这些机制可能包括对T细胞库选择的影响。

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