Your search keyword '"Turcant, Alain"' showing total 2 results

1. New evidence for oxetorone toxicity.

Author

Deguigne, Marie, Bruneau, Chloé, Touré, Ali, Turcant, Alain, and Le Roux, Gaël

Subjects

SEROTONIN, VENTRICULAR tachycardia, HYPOTENSION, CARDIOGENIC shock, SERUM

Abstract

Context:Oxetorone is a serotonin antagonist antimigraine drug but literature relating to its toxic properties is poor. The aim of this study is to describe the toxicological profile of oxetorone and to highlight any relationship between clinical and analytical findings. Materials and methods:This is a retrospective and observational study of cases exposure to oxetorone, reported to the Angers Poison and Toxicovigilance Centre between January 2002 and May 2016. Severity was assessed using the Poisoning Severity Score (PSS). Cases where data were incomplete, where oxetorone was deemed not accountable, where clinical signs were linked mainly to a co-ingested drug or where the plasma concentration of oxetorone was negative were all excluded. Results:We included 43 cases of exposure, 31 of whom were suicide attempts. The assumed ingested dose (60–3600 mg) was correlated to severity (rs = 0.45,p = 0.01). Symptoms of moderate severity (PSS2 = drowsiness, hypertonia, myosis, convulsions, arterial hypotension, QRS widening, QTc prolongation) were observed following ingestion of more than 600 mg of oxetorone (median dose =1200 mg) and severe symptoms (PSS 3 = coma, convulsions, QTc prolongation, QRS widening, ventricular tachycardia, arterial hypotension, cardiogenic shock) were observed starting from 1800 mg (median dose =2700 mg). In four cases, a secondary worsening of symptoms 10–48 h following ingestion was observed. Plasma oxetorone was measured in four patients. Severe symptoms were observed in the event of a concentration over 0.3 mg/L and the highest measured serum oxetorone level was delayed by 20–48 h following the ingestion for two cases. Conclusions:Several clinical and paraclinical parameters strongly point towards membrane-stabilising properties of the molecule and the risk of a delayed occurrence of symptoms or a secondary worsening. [ABSTRACT FROM PUBLISHER]

Published

2017

2. Cardiogenic shock and status epilepticus after massive bupropion overdose.

Author

Morazin, Florian, Lumbroso, Agnès, Harry, Patrick, Blaise, Marcel, Turcant, Alain, Montravers, Philippe, and Gauzit, Rémy

Subjects

EPILEPSY, ANTICONVULSANTS, TACHYCARDIA, CARDIOGENIC shock, DRUG overdose, HEART diseases

Abstract

Background. To describe a profound cardiac dysfunction and a status epilepticus after a massive bupropion overdose. Case report. A 35-year-old man was admitted in coma following the deliberate ingestion of 12 g of bupropion. The course was marked by the rapid onset of severe and prolonged status epilepticus and cardiogenic shock. Plasma bupropion level determined four hours after the estimated time of ingestion was 1.4 mg/L. All clinical features resolved completely in response to symptomatic treatment. Conclusion. Several cases of bupropion overdose, with sinus tachycardia and seizures rapidly corrected by symptomatic treatment, have been reported in the literature. To our knowledge, this case of overdose with bupropion alone, at very high doses, is the first to describe clinical features comprising severe and prolonged status epilepticus and direct cardiotoxicity with the development of cardiogenic shock documented by echocardiogram. [ABSTRACT FROM AUTHOR]

Published

2007