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Predictors of interstitial lung disease in early systemic sclerosis: a prospective longitudinal study of the GENISOS cohort

机译:早期系统性硬化中间质性肺疾病的预测因素:GENISOS队列的前瞻性纵向研究

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Introduction The objective of the present study was to examine the association of baseline demographic and clinical characteristics with sequentially obtained measurements of forced vital capacity (FVC), expressed as a percentage of the predicted value, and to identify predictors of the decline rate in FVC over time in the Genetics versus Environment in Scleroderma Outcome Study (GENISOS). Methods To date, 266 patients have been enrolled in GENISOS, a prospective, observational cohort of patients with early systemic sclerosis. In addition to pulmonary function tests (PFTs), clinical and laboratory data were obtained from each patient. We analyzed 926 FVC measurements utilizing generalized linear mixed models. The predictive significance of baseline variables for the decline rate in FVC was investigated by the interaction term between the variable and the follow-up time within the first 3 years after enrollment as well as throughout the entire follow-up time. Results The cohort consisted of 125 white, 54 African American, and 77 Hispanic patients with average disease duration of 2.5 years at enrollment. The mean follow-up time was 3.8 years, ranging up to 11.4 years. A number of baseline variables, including antibody status, African American ethnicity, disease type, baseline PFT values, modified Rodnan Skin Score, fibrosis on chest radiograph, and lung and skin subscores of the Severity Index, were associated with serially measured FVC levels. However, only the presence of anti-topoisomerase I antibodies (ATA) was associated with lower FVC levels (P 0.001) as well as accelerated decline rate in FVC within the first 3 years of follow-up (P = 0.02). None of the baseline variables predicted the rate of decline in FVC on long-term follow-up. Patients with rapidly progressive ILD, however, were under-represented in the long-term follow-up group because the accelerated rate of decline in FVC was associated with poor survival (P = 0.001). Conclusions Presence of ATA was the only baseline variable associated with differential FVC levels, predicting the rate of decline in FVC within the first 3 years of follow-up. The association of faster decline in FVC with poor survival further emphasizes the need for identification of predictive biomarkers by collection of genetic information and serial blood samples in cohort studies.
机译:引言本研究的目的是检查基线人口统计学特征和临床特征与依次获得的强制肺活量(FVC)的测量值(以预测值的百分比表示)之间的关系,并确定FVC下降率的预测因素。硬皮病结果研究(GENISOS)中遗传学与环境之间的差异。方法迄今为止,已有266名患者被纳入GENISOS,这是早期系统性硬化症患者的一项前瞻性观察性队列研究。除了肺功能测试(PFT),还从每位患者获得临床和实验室数据。我们使用广义线性混合模型分析了926个FVC测量值。基线变量对FVC下降率的预测意义通过变量与随访入组后三年内以及整个随访时间内的随访时间之间的交互项进行研究。结果该队列包括125名白人,54名非裔美国人和77名西班牙裔患者,入组时平均病程为2.5年。平均随访时间为3.8年,最长为11.4年。一系列基线变量,包括抗体状态,非裔美国人种族,疾病类型,基线PFT值,改良的Rodnan皮肤评分,胸部X线照片上的纤维化以及严重程度指数的肺和皮肤评分均与连续测量的FVC水平相关。但是,只有抗拓扑异构酶I抗体(ATA)的存在与较低的FVC水平(P <0.001)以及随访的前3年内FVC的加速下降速率有关(P = 0.02)。基线变量均未预测长期随访中FVC的下降率。但是,在长期随访组中,患有快速进行性ILD的患者代表性不足,因为FVC下降的加速速率与不良的生存率相关(P = 0.001)。结论ATA的存在是与差异性FVC水平相关的唯一基线变量,预测了随访的前三年内FVC的下降率。 FVC的快速下降与不良生存之间的关联进一步强调了在队列研究中需要通过收集遗传信息和连续血样来鉴定预测性生物标志物。

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