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首页> 外文期刊>The Journal of rheumatology >Patients chosen for treatment with cyclosporine because of severe rheumatoid arthritis are more likely to carry HLA-DRB1 shared epitope alleles, and have earlier disease onset.
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Patients chosen for treatment with cyclosporine because of severe rheumatoid arthritis are more likely to carry HLA-DRB1 shared epitope alleles, and have earlier disease onset.

机译:由于严重的类风湿性关节炎而选择用环孢霉素治疗的患者更有可能携带HLA-DRB1共有的表位等位基因,并且发病较早。

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OBJECTIVE: To determine whether patients with rheumatoid arthritis (RA) selected for treatment with cyclosporin A (CSA) because of severe disease are more likely to carry HLA-DRB1 alleles encoding the conserved "shared epitope" (SE) sequence. METHODS: The majority of patients (n = 178) were currently being treated with methotrexate (MTX), either alone or in combination with chloroquine and/or CSA. In about 30% of patients, treatment with CSA had been initiated because of limited response to MTX or MTX and chloroquine. Patients were treated as clinically indicated without knowledge of their HLA-DRB1 status. HLA-DRB1 typing was by a reverse dot blot method. RESULTS: Patients that had been treated with CSA were significantly more likely to carry an SE allele than patients not treated with CSA (81.5% vs 60.5%; OR 2.9, p = 0.006). Patients with 2 SE alleles were the most likely to have been treated with CSA. Results were still significant after correction for age, sex, and disease duration in a logistic regression model. There was no association between rheumatoid factor positivity and requirement for CSA therapy. Examination of individual SE alleles by multiple logistic regression analysis indicated that the strongest association was with presence of HLA-DRB1**0401 (p = 0.004). The DRB1*0401/*0404 genotype provided the greatest risk of requiring CSA treatment. Patients selected for CSA treatment had developed RA at a significantly earlier age than those not requiring CSA (44.4 vs 51.3 yrs; p = 0.004). CONCLUSION: Patients requiring treatment with CSA because of severe RA were significantly more likely to carry an SE allele than patients not requiring such treatment. CSA treated patients were also more likely to have had earlier age of disease onset. These data provide further evidence that bearing the SE (particularly 2 alleles) is associated with development of severe RA.
机译:目的:确定因严重疾病而选择用环孢菌素A(CSA)治疗的类风湿性关节炎(RA)患者是否更有可能携带编码保守的“共有表位”(SE)序列的HLA-DRB1等位基因。方法:大多数患者(n = 178)目前正在接受甲氨蝶呤(MTX)单独或与氯喹和/或CSA联合治疗。在大约30%的患者中,由于对MTX或MTX和氯喹的反应有限,已经开始使用CSA治疗。在不了解其HLA-DRB1状态的情况下,按照临床指示对患者进行了治疗。 HLA-DRB1分型是通过反向斑点印迹法进行的。结果:与未接受CSA治疗的患者相比,接受过CSA治疗的患者携带SE等位基因的可能性更高(81.5%vs 60.5%; OR 2.9,p = 0.006)。具有2个SE等位基因的患者最有可能接受CSA治疗。在逻辑回归模型中校正年龄,性别和疾病持续时间后,结果仍然很显着。类风湿因子阳性与CSA治疗需求之间没有关联。通过多重逻辑回归分析对单个SE等位基因的检查表明,最强的关联是与HLA-DRB1 ** 0401的存在有关(p = 0.004)。 DRB1 * 0401 / * 0404基因型提供了需要CSA治疗的最大风险。选择接受CSA治疗的患者比不需要CSA的患者显着更早出现RA(44.4岁对51.3岁; p = 0.004)。结论:由于严重的RA而需要接受CSA治疗的患者比不需要进行此类治疗的患者携带SE等位基因的可能性更高。 CSA治疗的患者也更可能具有较早的疾病发作年龄。这些数据提供了进一步的证据,证明带有SE(特别是2个等位基因)与严重RA的发展有关。

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