Search for predictors of achieving minimal disease activity during tofacitinib therapy in patients with psoriatic arthritis

L. D. Vorobyova, T. Korotaeva, S. Glukhova, E. Loginova, E. Gubar, Y. L. Korsakova
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Abstract

Objective: to search predictors of achieving minimal disease activity (MDA) during therapy in patients with psoriatic arthritis (PsA).Materials and methods. The study included 41 patients, predominantly men (58.9 %), with a confirmed PsA diagnosis and a disease duration of at least 6 months. In all cases, the diagnosis fulfilled the CASPAR criteria. The mean age of the patients at the time of enrolment in the study was 43.0±10.1 years, the duration of PsA was 7.7±7.1 years, the duration of psoriasis was 18.6±10.4 years, and the DAPSA index was 44.2±17.1. All patients were prescribed tofacitinib at a dose of 5 mg twice daily, followed by a possible dose increase to 10 mg twice daily. In addition to a general clinical examination and a standard rheumatological examination, the level of secreted DKK-1 protein and health-related quality of life (HRQoL, using a special PsAID-12 questionnaire) were determined. Multivariate stepwise discriminant analysis was used to search for predictors for the achievement of MDA in patients with PsA and to calculate the coefficients.Results and discussion. Based on the results obtained, a predictor for the achievement of MDA (PMDA) was developed: PMDA=-1.165 × number of inflamed entheses + DKK-1 level (pmol/l) + 3.086 × PsAID-12 “Skin lesions” scale value (if this indicator was ≤3 points, it was assigned a value of 1, if it was >3 points – 0) + 2.568 × PsAID-12 “Pain” scale (if this indicator was ≤6 points, it was assigned a value of 1, if it was >6 points – 0).The ROC analysis, which reflects the prognostic significance of this index, showed AUC (area under the curve) of 0.803 (95% confidence interval 0.739–0.867; p=0.02). PMDA=3.89 was chosen as the cut-off value; the sensitivity of this indicator was 91 %, the specificity – 79 %. Therefore with a PMDA ≥3.89, the probability of the patient achieving a MDA after 3 months is high; with a PMDA ˂ 3.89, it is low.Conclusion. We identified factors influencing the achievement of MDA in patients with PsA and developed a mathematical model. It allows timely assessment of the quality of treatment and its correction if necessary, thereby slowing disease progression.
寻找银屑病关节炎患者在接受托法替尼治疗期间达到最小疾病活动度的预测因素
目的:研究银屑病关节炎(PsA)患者在治疗期间达到最小疾病活动度(MDA)的预测因素。研究纳入了 41 名确诊为银屑病关节炎且病程至少 6 个月的患者,主要为男性(58.9%)。所有病例的诊断均符合 CASPAR 标准。患者入组时的平均年龄为(43.0±10.1)岁,PsA病程为(7.7±7.1)年,银屑病病程为(18.6±10.4)年,DAPSA指数为(44.2±17.1)。所有患者都接受了托法替尼治疗,剂量为 5 毫克,每天两次,之后剂量可能增加到 10 毫克,每天两次。除了一般临床检查和标准风湿病学检查外,还测定了分泌型DKK-1蛋白水平和健康相关生活质量(HRQoL,使用特殊的PsAID-12问卷)。采用多变量逐步判别分析寻找 PsA 患者达到 MDA 的预测因素并计算系数。根据所获得的结果,得出了MDA达标的预测因子(PMDA):PMDA=-1.165×发炎粘膜数量+DKK-1水平(pmol/l)+3.086×PsAID-12 "皮肤病变 "量表值(如果该指标≤3分,则赋值为1,如果>3分,则赋值为0)+2.568×PsAID-12 "皮肤病变 "量表值(如果该指标≤3分,则赋值为1,如果>3分,则赋值为0)。反映该指数预后意义的 ROC 分析显示,AUC(曲线下面积)为 0.803(95% 置信区间为 0.739-0.867;P=0.02)。选择 PMDA=3.89 作为临界值;该指标的敏感性为 91%,特异性为 79%。因此,当 PMDA≥3.89 时,患者在 3 个月后达到 MDA 的概率较高;当 PMDA ˂ 3.89 时,患者达到 MDA 的概率较低。我们确定了影响 PsA 患者达到 MDA 的因素,并建立了一个数学模型。我们确定了影响 PsA 患者达到 MDA 的因素,并建立了一个数学模型,从而可以及时评估治疗质量,并在必要时进行纠正,从而减缓疾病进展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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