Table 2.
Monitoring and referral to cardiology
| Cardiotoxicity risk | Monitoring |
|---|---|
| High risk drugs + established heart disease and LVEF <40% |
Carefully assess indication for cardiotoxic agents. Individualize, support from cardiology |
| High/moderate risk drugs + CVRF or LVEF >40% |
Baseline: ECG; blood test (HbA1c, lipids and troponin?); LVEF measurement (2D/3D US ± GLS) During treatment: control CVRF, troponin in each cycle?; assess BB, ACEIs, and statins End of treatment: troponin?; ECG, LVEF measurement (2D/3D US ± GLS) Follow-up: measure LVEF at 6 months from end of treatment (2D/3D US ± GLS), and every 3–4 years |
| High/moderate risk drugs + asymptomatic without CVRF |
Baseline: ECG; blood test (HbA1c, lipids, and troponin?) End of treatment: troponin?; ECG, LVEF measurement (2D/3D US ± GLS) Follow-up: according to symptoms |
| Criteria for referral to cardiology Patients with high or intermediate risk of cardiotoxicity, to optimize medical treatment: BB, ACEIs, statins Previous treatment with adriamycin ≥300 mg/m2 Mediastinal irradiation ≥30 Gy Previous heart disease (cardiomyopathy, heart failure, arrhythmias or ischemic heart disease), if not followed up in cardiology Poorly controlled CVRF with treatment: HT, diabetes, dyslipidemia, smoking Alterations at baseline: ECG, troponin or LVEF measurement Alterations during follow-up: LVEF decrease >10% or LVEF <53% Abnormal GLS (>−19%) or decrease >15% Positive troponin I Chest pain, dyspnea on exertion, syncope, arrhythmias HT refractory to conventional treatment | |
ACEIs angiotensin converting enzyme inhibitors, BB beta-blockers, CVRF cardiovascular risk factors, ECG electrocardiogram, GLS global longitudinal strain, Hb hemoglobin, HT hypertension, LVEF left ventricular ejection fraction