Complex and Severe Amiodarone-Induced Pleuro-Pulmonary Toxicity

Amiodarone is a class III antiarrhythmic agent widely used for the treatment of ventricular and supraventricular rhythm disorders [1,2]; its spectrum of toxicity is wide: thyroid, heart, lung, eye, skin, liver, gastrointestinal tract, and central nervous system [3]. All these effects are mediated by the mitochondrial toxicity of the drug and its lipophilicity. This toxicity is not dose-dependent, can occur even very early, and men seems to be more exposed than women [4]. The current incidence of amiodarone pneumonia is estimated at 1.6-2% [5,6]. His most classic presentation is acute or subacute pneumonia, while pleural involvement is exceptional [3,7] and often described as an unusual manifestation of amiodarone-induced pneumopathy [7,8]; similarly, acute hepatitis under amiodarone is very rare (<3%) [6]. We are reporting an original observation of triple toxicity to amiodarone with concomitant bilateral pleural, pulmonary parenchymal and hepatic involvement. Abstract Introduction: Pulmonary complications related to amiodarone have become exceptional with the doses currently used; their frequency is estimated at 1.6-2%. Acute or subacute pneumonia is the most classic manifestation. Pleural involvement under amiodarone is exceptional and unusual. We report an original observation of triple toxicity to amiodarone with concomitant pulmonary parenchymal, pleural and hepatic involvement and which was spontaneously resolved.


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Case Report 71-years-old patient, hypertensive and diabetic type 2, without degenerative complications, treated with amiodarone for four years for atrial fibrillation, was hospitalized because of severe acute pneumopathy evolving for ten days. The examination found apyretic patient, dyspneic (polypnea at 26 cycles/min and spontaneous oxygen saturation at 82%) with diffuse crepitant rales, bilateral pleuritis, and moderate hepatomegaly. The electrocardiogram showed slower atrial arrhythmia (mean frequency at 90/min) and the cardiac enzymes were not elevated. Chest X-ray showed bilateral and diffuse interstitial infiltrates ( Figure 1

Discussion
Although rarely observed, toxic pulmonary involvement caused by amiodarone is a major cause of discontinuation of this treatment [1,7,9]. Classically assessed at 5-7% [2,10], amiodaroneinduced pneumopathy appears to be clinically overestimated [5,6]. Indeed, in the large controlled and double-blind study, including 3439 patients receiving daily 400 mg or less amiodarone, pulmonary toxicity was noted only in 1.6% [5]. This pulmonary toxicity of amiodarone has been markedly reduced using lower doses of the drug but can occur with any dose [3]. Clinically, amiodarone-induced pneumopathy may manifest itself as: cough, chest discomfort, often progressive dyspnea, chest pain, and more rarely hemoptysis or acute respiratory failure in the exceptional forms of intra-alveolar haemorrhage or acute respiratory distress syndrome [2,9,11]. However, it can remain totally infra-clinical (insidious), and would only be found in pulmonary imaging [2,9,11]. Radiologically, this toxic pneumopathy may be in the form of: diffuse interstitial lung disease, acute or chronic organizing pneumonia, eosinophilic pneumonia, single or multiple nodules or mass-like lesions, desquamative interstitial pneumonia, and diffuse alveolar haemorrhage [3,11,12]. These lesions can be rapidly progressive [2] with the risk of irreversible pulmonary fibrosis [2,9,12]. Pleural effusion/pleurisy remains exceptional during amiodarone pulmonary toxicity [3,7,8]. It is classically bilateral and exudative [8,13]. It is rarely isolated [7], most often associated with parenchymal pulmonary toxicity or other toxic organ damage [8,13], and may exceptionally be, as in our observation, the first sign indicative of this toxicity [8,13]. Hepatic injury with amiodarone is rare and often unpredictable. Its frequency is estimated at 15-30% for elevated liver enzymes and less than 3% for acute hepatitis [6]. It can be irreversible in 50% of cases and even lead to severe forms of steatohepatitis with cirrhosis and portal hypertension [6]. Similarly, pulmonary involvement can also progress to irreversible fibrosis in 5 to 7% of cases [14] with a mortality estimated at 9% [2]. Treatment is based on discontinuation of the drug and, in severe cases, systemic corticosteroids for 4 to 12 months; the initial dose is 40-60mg/day followed by a gradual decline [3].
Corticosteroid therapy allows rapid improvement of pulmonary gas exchange and reversibility of radiological abnormalities [10].
Relapse after discontinuation of corticosteroid therapy has been reported mainly in obese subjects. Early detection of amiodaroneinduced pulmonary toxicity significantly improves its prognosis which can be fatal [2,9,12] (50% of cases if acute respiratory distress syndrome [2]), and clinical recommendations are currently well established for this [5,6].

Conclusion
The pulmonary toxicity of amiodarone has become rare with the use of lower doses; it can happen even early enough and with any dose. Regular clinical, radiological and biological monitoring makes it possible to detect and take these complications in time.
Our observation is characterized by the association of a triple toxicity with amiodarone: pulmonary, hepatic, and pleural which is exceptional, and by its spontaneous resolution. It is necessary to think of the iatrogenic cause due to amiodarone in front of any bilateral pleurisy that is not proven in patient under amiodarone.