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首页> 外文期刊>Rheumatic diseases clinics of North America >Prognostic use of human leukocyte antigen genotyping for rheumatoid arthritis susceptibility, disease course, and clinical stratification.
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Prognostic use of human leukocyte antigen genotyping for rheumatoid arthritis susceptibility, disease course, and clinical stratification.

机译:人类白细胞抗原基因分型在类风湿关节炎易感性,疾病过程和临床分层中的预后用途。

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HLA markers of the class II region are important for determination of the predisposition to RA, clinical manifestations, and rate of progression of joint destruction in this autoimmune disease. Furthermore, evidence emerges indicating that HLA markers also have an impact on treatment outcome in RA. Currently, several immunopathogenetic models of HLA-dependent influences in RA are under debate. These models insufficiently explain the graded influence of HLA-DR and HLA-DQ on manifestation and joint destruction, however. Currently, there is not enough evidence to unequivocally identify a primary susceptibility locus or to pinpoint the HLA-dependent mechanism in RA. Overall, the influence of HLA class II markers on disease susceptibility is rather restricted, and, in turn, their utility in establishing the diagnosis of RA is of limited use. Although relative risks are higher for the association of particular genotypes with extra-articular forms of RA, HLA genotyping may not contribute to prognostication in individual patients but may aid in disease stratification. In contrast, HLA genotyping in early RA, particularly when combined with the determination of RFs and determination of the presence of bony erosions, is of value to identify patients at risk for poor outcome. In turn, these patients may benefit from early aggressive therapy, and HLA genotyping should be useful to aid in risk stratification in patients and thus helpful for the choice of treatment. Lastly, disease and risk stratification based on HLA markers along with the elucidation of HLA-dependent mechanisms may facilitate the development of specific immunotherapy modalities.
机译:II类区域的HLA标记对于确定该自身免疫性疾病的RA易感性,临床表现以及关节破坏的进展速度非常重要。此外,有证据表明HLA标记物也对RA的治疗结果有影响。当前,关于RA中HLA依赖性影响的几种免疫病理模型正在争论中。但是,这些模型不足以解释HLA-DR和HLA-DQ对表现和关节破坏的分级影响。当前,没有足够的证据明确地确定主要的易感基因座或查明RA中HLA依赖性机制。总体而言,HLA II类标志物对疾病易感性的影响相当有限,因此,它们在建立RA诊断中的用途有限。尽管将特定基因型与关节外形式的RA关联起来的相对风险较高,但HLA基因分型可能无助于个别患者的预后,但可能有助于疾病分层。相比之下,早期RA中的HLA基因分型,特别是与RF的确定和骨侵蚀的存在相结合时,对于识别处于不良预后风险中的患者非常有价值。反过来,这些患者可能会从早期积极治疗中受益,HLA基因分型应有助于患者的风险分层,从而有助于选择治疗方法。最后,基于HLA标记的疾病和风险分层以及对HLA依赖机制的阐明可能有助于开发特定的免疫疗法。

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