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首页> 外文期刊>The Journal of rheumatology >Immunogenetic risks of anti-cyclical citrullinated peptide antibodies in a North American Native population with rheumatoid arthritis and their first-degree relatives.
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Immunogenetic risks of anti-cyclical citrullinated peptide antibodies in a North American Native population with rheumatoid arthritis and their first-degree relatives.

机译:抗环瓜氨酸肽抗体在类风湿性关节炎的北美原住民及其一级亲属中的免疫遗传风险。

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OBJECTIVE: To determine the prevalence of anti-cyclic citrullinated peptide (anti-CCP) antibodies in unaffected relatives of North American Native probands with rheumatoid arthritis (RA); and the associations of the shared epitope (SE) and HLA-DRB1*0901 with RA and anti-CCP antibodies. METHODS: The subjects were RA probands, affected relatives, unaffected first-degree (FDR) and more distant relatives, and unaffected controls from the same population. HLA-DRB1 typing was determined by DNA sequencing and anti-CCP antibodies were determined by ELISA. RESULTS: DRB1*0901, SE, and SE/DRB1*0901 genotypes were all associated with RA. SE/DRB1*0901, but not other SE genotypes, was associated with disease onset at age<16 years. The frequency of anti-CCP antibodies was 82% in RA probands, 17% in FDR, 11% in more distant relatives, and 3% in controls. Among unaffected relatives, a significant increased risk of anti-CCP was associated with SE/DRB1*0901 genotype, but not with SE. CONCLUSION: An independent association of the non-SE allele DRB1*0901 with RA was confirmed in this population, and this allele in combination with a SE allele was associated with younger age at disease onset. FDR of RA probands have a higher prevalence of anti-CCP antibodies than more distant relatives and unrelated controls, suggesting a gradient of risk for disease development. Immunogenetic risks may act early in disease pathogenesis at the level of initiation of RA autoantibody formation; however, it is not clear what additional genetic and environmental risks are involved in progression to clinical disease.
机译:目的:确定抗环瓜氨酸肽(anti-CCP)抗体在未患风湿性关节炎(RA)的北美原住民先证者的亲属中的患病率;以及共享表位(SE)和HLA-DRB1 * 0901与RA和抗CCP抗体的关联。方法:受试者为RA先证者,受影响的亲戚,未受影响的一级(FDR)和较远的亲戚,以及同一人群中未受影响的对照。通过DNA测序确定HLA-DRB1的类型,并通过ELISA确定抗CCP抗体。结果:DRB1 * 0901,SE和SE / DRB1 * 0901基因型均与RA相关。 SE / DRB1 * 0901与其他SE基因型无关,但与16岁以下的疾病发作有关。抗CCP抗体的频率在RA先证者中为82%,在FDR中为17%,在较远的亲戚中为11%,在对照组中为3%。在未受影响的亲戚中,抗CCP的风险显着增加与SE / DRB1 * 0901基因型相关,而与SE无关。结论:在该人群中证实了非SE等位基因DRB1 * 0901与RA的独立关联,并且该等位基因与SE等位基因结合与发病年龄较小有关。与较远的亲戚和无关亲戚相比,RA先证者的FDR患抗CCP抗体的患病率更高,表明疾病发展的风险梯度有所提高。免疫原性风险可能在RA自身抗体形成起始水平的疾病发病机理中起作用;但是,尚不清楚在临床疾病进展中还涉及哪些其他遗传和环境风险。

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