间质性肺疾病的治疗负担：经验教训。

Therapeutic burden in interstitial lung disease: Lessons to learn.

机构信息

Department of Respiratory and Sleep Medicine, Austin Health, Melbourne, VIC, Australia.

Institute for Breathing and Sleep, Melbourne, VIC, Australia.

出版信息

Respirology. 2019 Jun;24(6):566-571. doi: 10.1111/resp.13480. Epub 2019 Feb 20.

DOI:10.1111/resp.13480

PMID:30790404

Abstract

BACKGROUND AND OBJECTIVE

Patients with interstitial lung disease (ILD) are often prescribed disease-targeted and symptomatic therapies, both of which can cause significant treatment burden due to polypharmacy and drug-disease interactions. This study aimed to evaluate medication regimen complexity before and after introduction of ILD-specific therapies. Potential drug-disease interactions were evaluated for patients who were prescribed prednisolone.

METHODS

In this study, 214 patients with ILD were assessed for demographic information, co-morbidities and medication use. Medication lists were reviewed prior to and after the introduction of ILD-specific therapies. Complexity of treatment regimen was examined using the validated Medication Regimen Complexity Index (MRCI).

RESULTS

Of the 214 patients, 75 had idiopathic pulmonary fibrosis (IPF) while the rest had inflammatory ILD (chronic hypersensitivity pneumonitis: 45; connective tissue disease-related ILD: 41). Polypharmacy was common at baseline (IPF: 51%, inflammatory ILD: 63%). Following introduction of ILD-specific therapies, median total MRCI scores significantly increased from 8 (interquartile range (IQR) = 8-15) to 22.5 (17.5-27.5) and 14.5 (8.5-21) to 21.5 (16-30) for IPF and inflammatory ILD groups, respectively (P < 0.0001 for both). Complex dosing instructions contributed the most to total MRCI scores for ILD-specific therapies. Among patients receiving prednisolone (n = 113), 88% had ≥1 co-morbidity which may be impacted. Common co-morbidities included gastrointestinal diseases (56%), obesity (37%), osteoporosis (24%) and diabetes mellitus (18%).

CONCLUSION

Polypharmacy and complex medication regimen are common in patients with ILD of different aetiologies. There is a high frequency of potential drug-disease interactions among patients who are prescribed systemic corticosteroids. These findings highlight the need for careful evaluation of the impact of therapeutic complexity and burden in patients with ILD.

摘要

背景与目的

间质性肺疾病（ILD）患者通常接受靶向疾病和对症治疗，由于多种药物治疗和药物-疾病相互作用，这两种治疗都会带来显著的治疗负担。本研究旨在评估ILD 特异性治疗前后药物治疗方案的复杂性。对于接受泼尼松龙治疗的患者，评估了潜在的药物-疾病相互作用。

方法

本研究评估了 214 例ILD 患者的人口统计学信息、合并症和药物使用情况。在ILD 特异性治疗引入前后，对药物清单进行了审查。使用经过验证的药物治疗方案复杂性指数（MRCI）来检查治疗方案的复杂性。

结果

214 例患者中，75 例为特发性肺纤维化（IPF），其余为炎症性ILD（慢性过敏性肺炎：45 例；结缔组织病相关ILD：41 例）。基线时合并用药很常见（IPF：51%，炎症性ILD：63%）。ILD 特异性治疗引入后，IPF 和炎症性ILD 组的中位总 MRCI 评分分别从 8（四分位距（IQR）= 8-15）显著增加至 22.5（17.5-27.5）和 14.5（8.5-21）至 21.5（16-30）（均 P < 0.0001）。复杂的给药说明对ILD 特异性治疗的总 MRCI 评分贡献最大。在接受泼尼松龙治疗的 113 例患者中，88%有≥1 种合并症可能受到影响。常见的合并症包括胃肠道疾病（56%）、肥胖（37%）、骨质疏松症（24%）和糖尿病（18%）。