Boehringer Ingelheim, Ridgefield, Connecticut.
Optum, Eden Prairie, Minnesota; and.
Ann Am Thorac Soc. 2022 Jul;19(7):1112-1121. doi: 10.1513/AnnalsATS.202102-222OC.
Chronic fibrosing interstitial lung disease (ILD) with a progressive phenotype is a clinical concept describing the broad group of ILDs characterized by progressive pulmonary fibrosis. The prevalence of progressive fibrotic ILDs other than idiopathic pulmonary fibrosis (IPF) is not well understood. We used a novel algorithm to estimate the prevalence range of disease progression among patients with non-IPF fibrotic ILD in a U.S. claims database. This was a retrospective study including adults with commercial or Medicare Advantage with Part D (MAPD) insurance using administrative claims data from October 2015 to September 2019. Patients likely to have non-IPF fibrosing ILD with a progressive phenotype were identified via an algorithm that incorporated ILD-related diagnosis codes (excluding IPF) and claims-based proxies for fibrotic ILD progression, including pulmonary function tests, chest imaging, oral corticosteroid (OCS) medications, immunosuppressive medications, lung transplant, oxygen therapy, palliative care, and respiratory hospitalization. The prevalence range of non-IPF fibrotic ILD with progressive disease behavior was calculated using strict and lenient case definitions to account for potential imprecision in the progression proxies. Of nearly 9 million study-eligible patients, 17,136 were identified with non-IPF fibrosing ILD. The prevalence of disease progression per 10,000 (95% confidence interval) ranged from 12.14 (11.74-12.54) to 29.05 (28.43-29.67) over a mean observation time of 1.44 years for MAPD enrollees ( = 14,686), and from 0.89 (0.81-0.97) to 2.36 (2.24-2.48) over a mean observation time of 1.29 years for commercial enrollees ( = 2,450). Prevalence estimates increased with age for both insurance types. Among patients with progression, 4,097 met at least two progression proxies not considering OCS (strict case definition) and 9,946 met at least one progression proxy (lenient case definition). The mean (standard deviation) number of proxies met was 2.1 (1.3), and the most common individual proxies met (alone or in combination with other proxies) were OCS use (48.9%), respiratory hospitalization (44.2%), and oxygen therapy (44.1%). This is among the first claims-based estimates of the prevalence of non-IPF chronic fibrosing ILD with a progressive phenotype. Our analysis indicates that this phenotype is rare in the overall population but increases substantially with increasing age.
慢性纤维性间质性肺病(ILD)具有进行性表型,是一种临床概念,描述了一组以进行性肺纤维化为特征的ILD。除特发性肺纤维化(IPF)以外的进行性纤维化ILD 的患病率尚不清楚。我们使用一种新的算法来估计美国索赔数据库中非 IPF 纤维性ILD 患者疾病进展的患病率范围。这是一项回顾性研究,纳入了使用商业或 Medicare Advantage with Part D(MAPD)保险的成年人的行政索赔数据,时间范围为 2015 年 10 月至 2019 年 9 月。通过一种算法识别出可能患有进行性表型非 IPF 纤维性 ILD 的患者,该算法纳入了ILD 相关的诊断代码(不包括 IPF)和基于索赔的纤维化 ILD 进展的替代指标,包括肺功能检查、胸部成像、口服皮质类固醇(OCS)药物、免疫抑制药物、肺移植、氧疗、姑息治疗和呼吸住院治疗。使用严格和宽松的病例定义计算非 IPF 纤维性ILD 进行性疾病行为的患病率范围,以考虑到进展替代指标的潜在不精确性。在近 900 万符合研究条件的患者中,有 17136 人被诊断为非 IPF 纤维性 ILD。在 MAPD 参保者( = 14686 人)的平均观察时间为 1.44 年和商业参保者( = 2450 人)的平均观察时间为 1.29 年的情况下,每 10000 人(95%置信区间)的疾病进展患病率范围从 12.14(11.74-12.54)到 29.05(28.43-29.67)不等。患病率估计随两种保险类型的年龄增长而增加。在进展的患者中,有 4097 人符合至少两个不考虑 OCS 的进展替代指标(严格病例定义),9946 人符合至少一个进展替代指标(宽松病例定义)。符合的替代指标的平均值(标准差)为 2.1(1.3),最常见的单独替代指标(单独或与其他替代指标结合)是 OCS 使用(48.9%)、呼吸住院治疗(44.2%)和氧疗(44.1%)。这是基于索赔的非 IPF 慢性纤维性ILD 进行性表型患病率的首批估计之一。我们的分析表明,这种表型在总体人群中很少见,但随着年龄的增长而显著增加。
