Bothrops lanceolatus Envenoming in Martinique: A Historical Perspective of the Clinical Effectiveness of Bothrofav Antivenom Treatment

Author:

Resiere Dabor12ORCID,Florentin Jonathan12,Mehdaoui Hossein12,Kallel Hatem3,Legris-Allusson Veronique4,Gueye Papa12ORCID,Neviere Remi12ORCID

Affiliation:

1. Department of Critical Care Medicine, Toxicology and Emergency, CHU Martinique (University Hospital of Martinique), 97200 Fort-de-France, France

2. Cardiovascular Research Team UR5_3 PC2E Pathologie Cardiaque, Toxicité Environnementale et Envenimations, Université des Antilles, 97233 Fort-de-France, France

3. Intensive Care Unit, Cayenne General Hospital, 97306 Cayenne, France

4. Department of Pharmacology, CHU Martinique (University Hospital of Martinique), 97200 Fort-de-France, France

Abstract

Bothrofav, a monospecific antivenom, was introduced in June 1991 and has shown excellent effectiveness against life-threatening and thrombotic complications of Bothrops lanceolatus envenoming. Because of the reoccurrence of cerebral stroke events despite the timely administration of antivenom, new batches of Bothrofav were produced and introduced into clinical use in January 2011. This study’s aim was to evaluate the effectiveness of Bothrofav generations at treating B. lanceolatus envenoming. During the first period of the study (2000–2010), 107 patients were treated with vials of antivenom produced in June 1991, while 282 envenomed patients were treated with vials of antivenom produced in January 2011 in the second study period (2011–2023). Despite timely antivenom administration, thrombotic complications reoccurred after an interval free of thrombotic events, and a timeframe analysis suggested that the clinical efficacy of Bothrofav declined after it reached its 10-year shelf-life. In of the case of an antivenom shortage due to the absence of regular batch production, no adverse effects were identified before the antivenom reached its 10-year shelf-life, which is beyond the accepted shelf-life for a liquid-formulation antivenom. While our study does not support the use of expired antivenom for potent, life-threatening B. lanceolatus envenoming, it can be a scientific message to public entities proving the necessity of new antivenom production for B. lanceolatus envenoming.

Funder

Agence Nationale de la Recherche

Publisher

MDPI AG

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