吡非尼酮胶囊或片剂在法国 RaDiCo-ILD 队列真实世界研究中的特发性肺纤维化治疗。

Treatment of Idiopathic Pulmonary Fibrosis with Capsule or Tablet Formulations of Pirfenidone in the Real-Life French RaDiCo-ILD Cohort.

机构信息

Pneumology Department, Center for Rare Pulmonary Diseases, Lyon Civil Hospices-Claude Bernard Lyon University-East Hospital Group-Louis Pradel Hospital, 59 Boulevard Pinel, Lyon, 69677, BRON Cedex, France.

Inserm-RaDiCo, Paris, France.

出版信息

Adv Ther. 2022 Jan;39(1):405-420. doi: 10.1007/s12325-021-01961-x. Epub 2021 Nov 10.

DOI:10.1007/s12325-021-01961-x

PMID:34757602

Abstract

INTRODUCTION

Pirfenidone, an antifibrotic medication for idiopathic pulmonary fibrosis (IPF), is now available in France in two formulations: tablets since April 2018, and the initial capsules form. We conducted a cohort study to describe tolerance and acceptability of capsules and/or tablets of pirfenidone in patients with IPF.

METHODS

This study was nested within the French, non-randomized, multicenter RaDiCo-ILD (Rare Disease Cohort-Interstitial Lung Diseases). Included patients with IPF received at least one dose of pirfenidone tablets or capsules from July 2017 to June 2019 in three populations: the inclusion population (patients treated at least once with pirfenidone during the study period, n = 288); the potential switch population (patients treated with pirfenidone during the switch period starting April 2018, n = 256); the newly treated population (patients who initiated pirfenidone during the study period, n = 162). Each of those last two populations included three subgroups (tablets, capsules, and substitution).

RESULTS

In 288 patients treated, 162 newly initiated pirfenidone during the study period: there were no meaningful differences in the baseline characteristics with the 256 patients treated during the potential switch period. In the newly treated population, 30.3% started pirfenidone treatment with tablet formulation. In the potential switch population, 44.9% of patients shifted from capsule to tablet. Half of the patients shifted to tablet formulation within the first 10 months. The mean treatment duration was 21.5 months with a mean dose of 2106.7 mg/day; 46.5% of patients discontinued treatment, mainly because of adverse events. There were fewer discontinuations in the tablets and substitution subgroups than in the capsules-only subgroup. The most reported adverse event was skin rash (11.5%). No new adverse event was identified.

CONCLUSIONS

This real-life cohort assessing the characteristics of the prescription of pirfenidone tablets and capsules suggests a good acceptability of the tablet formulation by patients with IPF.

TRIAL REGISTRATION

Clinical trial registered with www.clinicaltrials.gov (NCT04238871).

摘要

简介

吡非尼酮是一种治疗特发性肺纤维化 (IPF) 的抗纤维化药物，自 2018 年 4 月以来在法国以片剂和初始胶囊形式供应。我们进行了一项队列研究，以描述 IPF 患者使用吡非尼酮胶囊和/或片剂的耐受性和可接受性。

方法

这项研究是嵌套在法国、非随机、多中心 RaDiCo-ILD（罕见病队列-间质性肺疾病）中的。2017 年 7 月至 2019 年 6 月期间，至少接受过一次吡非尼酮治疗的患者被纳入包括人群（n=288）；潜在转换人群（在 2018 年 4 月开始的转换期间接受过吡非尼酮治疗的患者，n=256）；新治疗人群（在研究期间开始接受吡非尼酮治疗的患者，n=162）。后两个人群中的每一个都包括三个亚组（片剂、胶囊和替代）。

结果

在 288 名接受治疗的患者中，有 162 名在研究期间新开始使用吡非尼酮：在潜在转换期间接受治疗的 256 名患者的基线特征没有明显差异。在新治疗人群中，30.3%的患者开始使用片剂形式的吡非尼酮治疗。在潜在转换人群中，44.9%的患者从胶囊转换为片剂。一半的患者在头 10 个月内转换为片剂。平均治疗持续时间为 21.5 个月，平均剂量为 2106.7mg/天；46.5%的患者停止治疗，主要是因为不良反应。片剂和替代亚组的停药率低于仅胶囊亚组。报告最多的不良反应是皮疹（11.5%）。没有发现新的不良反应。