医院间特发性肺纤维化急性加重症患者的治疗实践和结局的差异:一项回顾性多中心队列研究。
Hospital-level variation in practices and outcomes for patients with severe acute exacerbations of idiopathic pulmonary fibrosis: a retrospective multicentre cohort study.
机构信息
Pulmonary Center, Boston University School of Medicine, Boston, Massachusetts, USA
Pulmonary Center, Boston University School of Medicine, Boston, Massachusetts, USA.
出版信息
BMJ Open Respir Res. 2023 Apr;10(1). doi: 10.1136/bmjresp-2022-001593.
BACKGROUND
In the absence of evidence-based strategies to improve patient outcomes, the management of patients with severe idiopathic pulmonary fibrosis (IPF) exacerbations may vary widely across centres. We assessed between-hospital variation in practices and mortality for patients with severe IPF exacerbations.
METHODS
Using the Premier Healthcare Database from 1 October 2015 to 31 December 2020, we identified patients admitted to intensive care unit (ICU) or intermediate care unit with an IPF exacerbation. We assessed idiosyncratic, between-hospital variation in ICU practices (invasive mechanical ventilation (IMV), non-invasive mechanical ventilation (NIMV), corticosteroid use, and immunosuppressive and/or antioxidant use) and hospital mortality by determining median risk-adjusted hospital rates and intraclass correlation coefficients (ICCs) from hierarchical multivariable regression models. A priori, an ICC>15% was deemed 'high variation'.
RESULTS
We identified 5256 critically ill patients with a severe IPF exacerbation at 385 US hospitals. Hospital median risk-adjusted rates of practices were: IMV (14% (IQR: 8.3%-26%)), NIMV (42% (31%-54%)), corticosteroid use (89% (84%-93%)), and immunosuppressive and/or antioxidant use (3.3% (1.9%-5.8%)). Model ICCs were: IMV (19% (95% CI: 18% to 21%)), NIMV (15% (13% to 16%)), corticosteroid use (9.8% (8.3% to 11%)), and immunosuppressive and/or antioxidant use (8.5% (7.1% to 9.9%)). The median risk-adjusted hospital mortality was 16% (IQR: 11%-24%) with an ICC of 7.5% (95% CI: 6.2% to 8.9%).
INTERPRETATION
We observed high variation in the use of IMV and NIMV, and less variation in corticosteroid and immunosuppressant and/or antioxidant use among patients hospitalised with severe IPF exacerbations. Further research is needed to guide the decisions surrounding initiation of IMV and role of NIMV and to understand the effectiveness of corticosteroids among patients with severe IPF exacerbations.
背景
在缺乏改善患者预后的循证策略的情况下,严重特发性肺纤维化(IPF)加重患者的管理可能因中心而异。我们评估了严重 IPF 加重患者的医院间实践和死亡率差异。
方法
我们使用 2015 年 10 月 1 日至 2020 年 12 月 31 日期间的 Premier Healthcare Database,确定了入住重症监护病房(ICU)或中级护理病房的 IPF 加重患者。我们通过确定分层多变量回归模型中的中位风险调整后的医院比率和组内相关系数(ICC),评估了 ICU 实践(有创机械通气(IMV)、无创机械通气(NIMV)、皮质类固醇使用、免疫抑制和/或抗氧化剂使用)和医院死亡率的医院间固有差异。事先规定,ICC>15%被认为是“高度变异”。
结果
我们在 385 家美国医院确定了 5256 名患有严重 IPF 加重的重症患者。实践的医院中位风险调整率为:IMV(14%(IQR:8.3%-26%))、NIMV(42%(31%-54%))、皮质类固醇使用(89%(84%-93%))和免疫抑制和/或抗氧化剂使用(3.3%(1.9%-5.8%))。模型 ICC 分别为:IMV(19%(95%CI:18%至 21%))、NIMV(15%(13%至 16%))、皮质类固醇使用(9.8%(8.3%至 11%))和免疫抑制和/或抗氧化剂使用(8.5%(7.1%至 9.9%))。中位风险调整后的医院死亡率为 16%(IQR:11%-24%),ICC 为 7.5%(95%CI:6.2%至 8.9%)。
解释
我们观察到严重 IPF 加重患者中 IMV 和 NIMV 的使用存在高度差异,而皮质类固醇和免疫抑制剂和/或抗氧化剂的使用差异较小。需要进一步研究来指导 IMV 启动决策以及 NIMV 的作用,并了解严重 IPF 加重患者中皮质类固醇的疗效。
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