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Natural variability in the disease course of SSc-ILD: implications for treatment

机译:SSC-ILD疾病过程中的自然变异:治疗的含义

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Interstitial lung disease (ILD) affects approximately 50% of patients with systemic sclerosis (SSc) and is the leading cause of death in SSc. Our objective was to gain insight into the progression of SSc-associated ILD (SSc-ILD). Using data from longitudinal clinical trials and observational studies, we assessed definitions and patterns of progression, risk factors for progression, and implications for treatment. SSc-ILD progression was commonly defined as exceeding specific thresholds of lung function worsening and/or increasing radiographic involvement. One definition used in several studies is decline in forced vital capacity (FVC) of ≥10%, or ≥5–10% plus a decline in diffusing capacity of the lung for carbon monoxide ≥15%. Based on these criteria, 20–30% of patients in observational cohorts develop progressive ILD, starting early in the disease course and progressing at a highly variable rate. Risk factors such as age, FVC, extent of fibrosis and presence of anti-topoisomerase I antibodies can help predict progression of SSc-ILD, though composite risk scores may offer greater predictive power. Whilst the variability of the disease course in SSc-ILD makes risk stratification of patients challenging, the decision to initiate, change or stop treatment should be based on a combination of the current disease state and the speed of progression.
机译:间质肺病(ILD)影响大约50%的系统性硬化症患者(SSC),是SSC中死亡的主要原因。我们的目标是深入了解SSC相关的ILD(SSC-ILD)的进展。使用来自纵向临床试验和观察研究的数据,我们评估了进展的定义和模式,危险因素的进展,以及治疗的影响。 SSC-ILD进展通常定义为超过肺功能恶化和/或增加射线照相的特定阈值。在几项研究中使用的一种定义是强制生气能力(FVC)下降≥10%,或≥5-10%,加上一氧化碳肺部扩散能力的下降≥15%。基于这些标准,20-30%的观察队列患者在疾病课程早期开始,从疾病课程开始,并以高度可变的速度进展。危险因素如年龄,FVC,纤维化的程度和抗拓甲异构酶I抗体的存在可以有助于预测SSC-ILD的进展,但综合风险评分可以提供更大的预测力。虽然SSC-ILD中疾病课程的可变性使得患者挑战的风险分层,但决定发起,改变或停止治疗应基于目前疾病状态和进展速度的组合。

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