Kardiotoxische Substanzen in der Onkologie: Was ist zu beachten?

 

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Zusammenfassung

Kardiale Nebenwirkungen von klassischen oder „molecular targeted“-Chemotherapien umfassen myokardiale Dysfunktion oder Kardiomyopathie, Koronartoxizität, Arrhythmien und arterielle Hypertonie. Die Myokardtoxizität als wichtigste Nebenwirkung kann in Typ I (permanent, direkte Myozytennekrosen; klassischer Vertreter Anthrazykline) und Typ II (reversibel, keine Nekrosen; klassischer Vertreter Trastuzumab) unterschieden werden. Eine Früherkennung einer subklinischen Myokardschädigung scheint mittels Speckle-Tracking-Echokardiografie und Troponin-Bestimmungen möglich. Effektive präventive und therapeutische Ansätze zur Minderung der Myokardtoxizität von Anthrazyklinen (verlängerte Infusion, liposomales Doxorubicin, Dexrazoxane, Betablocker, ACE-Hemmer) und von Trastuzumab (Betablocker, ACE-Hemmer) sind verfügbar. Aufgabe des sich entwickelnden Feldes der Kardioonkologie ist die Herstellung einer vernünftigen Balance zwischen onkologischer Effektivität und kardialen Risiken.

Abstract

Cardiac side effects of classical or molecular targeted chemotherapy include myocardial dysfunction or cardiomyopathy, coronary toxicity, arrhythmias and arterial hypertension. Myocardial toxicity can be permanent (type I: myocyte necrosis, typically induced by anthracyclines) or reversible (type II: no myocyte necrosis, typically induced by trastuzumab). Early detection of subclinical myocardial damage may be possible using speckle tracking echocardiography or troponin measurements. Effective preventive and therapeutic strategies to reduce the myocardial toxicity of anthracyclines (prolonged infusion time, liposomal doxorubicin, dexrazoxane, beta-blockers, ACE-inhibitors) and of trastuzumab (beta-blockers, ACE-inhibitors) are available. The evolving field of cardio-oncology has to define the reasonable balance between oncological effectiveness and cardiac risks of modern cancer chemotherapy.

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