Differential Effects of Pirfenidone on Acute Pulmonary Injury and Ensuing Fibrosis in the Hamster Model of Amiodarone-Induced Pulmonary Toxicity

doi:10.1093/toxsci/kfg167

ToxSci Advance Access originally published online on June 27, 2003

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Toxicological Sciences 75, 169-180 (2003)
Copyright © 2003 by the Society of Toxicology

RESPIRATORY TOXICOLOGY

Differential Effects of Pirfenidone on Acute Pulmonary Injury and Ensuing Fibrosis in the Hamster Model of Amiodarone-Induced Pulmonary Toxicity

Jeffrey W. Card^*, William J. Racz^*, James F. Brien^*, Solomon B. Margolin and Thomas E. Massey^*^,1

^* Department of Pharmacology and Toxicology, Queen’s University, Kingston, Ontario, Canada K7L 3N6, and Marnac Inc., Dallas, Texas 75231

Pulmonary toxicity, including fibrosis, is a serious adverseeffect associated with the antidysrhythmic drug amiodarone (AM).We tested the potential usefulness of pirfenidone against AM-inducedpulmonary toxicity in the hamster model. Intratracheal AM administrationresulted in pulmonary fibrosis 21 days posttreatment, as evidencedby an increased hydroxyproline content and histological damage.Dietary pirfenidone administration (0.5% w/w in chow), for 3days prior to and continuously after AM, prevented fibrosisand suppressed elevation of pulmonary transforming growth factor(TGF)-ß₁ mRNA content at 7 and 21 days post-AM. Protectionagainst AM-induced lung damage was not observed when supplementationwith pirfenidone was delayed until 7 days following AM administration,suggesting that alteration of early events in AM lung toxicityis necessary for the protective effect of pirfenidone. BothAM and bleomycin, another pulmonary fibrogen, caused inflammation24 h after intratracheal dosing, measured as increased lactatedehydrogenase activity, protein content, and cellular alterationsin bronchoalveolar lavage fluid, with the response to AM markedlygreater than that to bleomycin. Administration of AM, but notbleomycin, also caused whole lung mitochondrial dysfunction,alveolar macrophage death, and an influx of eosinophils intothe lung, of which pirfenidone was able to decrease only thelatter. We conclude that: (1) AM induces alveolar macrophagedeath and severe, acute pulmonary inflammation with associatedeosinophilia following intratracheal administration; (2) mitochondrialdysfunction may play an early role in AM pulmonary injury; and(3) pirfenidone decreases AM-induced pulmonary fibrosis in thehamster, probably through suppression of TGF-ß₁ geneexpression.

Key Words: amiodarone; pirfenidone; lung; inflammation; fibrosis; mitochondria.

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