CHIMIOTHERAPIE ET CARDIOTOXICITE

C. Brestescher, P. Pautier, D. Farge

Résultats de recherche: Contribution à un journalBrève enquêteRevue par des pairs

12 Citations (Scopus)

Résumé

Among the various anticancer drugs, used alone or in combination during courses of chemotherapy, anthracyclines (leader: doxorubicin) are responsible for direct myocardial toxicity, which can exceptionally be acute, but more often chronic with a delayed onset. This cardiotoxicity is directly proportional to the cumulative dose administered and the recommended total dose for doxorubicin is 550 mg/m2. The risk factors able to potentiate cardiotoxicity must be analysed before starting chemotherapy and follow-up by ultrasonography and/or isotope ejection fraction must be repeated before each course. The treatment of anthracycline-induced heart failure consists of digitalis alka[oids combined with angiotensin converting enzyme; inhibitors. The cardiac toxicity of 5FU is currently explained by the theory of coronary spasm; based on clinical findings such as chest pain associated with ischaemic electrical modifications. The incidence of this toxicity is low, but it can be fatal. Exceptional examples include the cardiotoxicity induced by high-dose cyclophosphamide responsible for acute haemorrhagic myocarditis, potentiation of the cardiotoxic effect of anthracyclines by dacarbazine and plicamycin, and serious ventricutal and supraventricular arrhythmias induced by amsacrine. Among the various cytokines used in oncology, interferon is responsible for heart failure, reversible after stopping treatment, but also for ventricular arrhythmias, or even sudden death, the pathophysiology of which still remains unclear.

Titre traduit de la contributionChemotherapy and cardiotoxicity
langue originaleFrançais
Pages (de - à)443-447
Nombre de pages5
journalAnnales de Cardiologie et d'Angeiologie
Volume44
Numéro de publication8
étatPublié - 1 janv. 1995
Modification externeOui

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