The study is multicenter, post-authorization, observational and ambispective
Cardiovascular toxicity produced by antitumoral drugs has a considerable impact in life wellness and prognosis of cancer patients, which can imply the suspension of the desired antitumoral treatment or even risk the patient´s life. The development of a risk score for these patients, as well as specific methodology for early detection of cardiotoxicity would therefore be a great outcome to trigger new strategies for the monitoring of these patients. Currently there is a lack of a clinical score to predict cardiotoxicity risk. Therefore, there is an urgent need to identify new myocardial injury biomarkers and novel imaging parameters for measuring ventricular function that would increase the sensitivity of the traditional methods used for the early detection of cardiotoxicity. The objectives of the present study are the following: * Identify the factors related with cardiotoxicity risk produced by antitumoral drugs. * Assess the utility of clinical, biological and functional parameters for the early detection of cardiotoxicity produced by antitumoral drugs. The study is a multicenter one, observational and ambispective. We will include all the patients assessed by the Oncology and Haematology Departments in each participant hospital that are about to initiate or are undergoing chemotherapy with any of the drugs specified in the study protocol. Patients will be monitorized during the treatment, undergoing an echocardiography study and a blood sample collection in each clinical timepoint. All these parameters will hopefully shed some light for the development of a clinical risk score as well as identifying new early biomarkers for cardiotoxicity. The initial follow-up in this phase of the study will be 2 years
Study Type
OBSERVATIONAL
Enrollment
3,400
La pAz University Hospital
Madrid, Madrid, Spain
RECRUITINGChange in CARDIOTOXICITY DEVELOPMENT RISK SCORE
Risk of cardiovascular toxicity by antitumoral agents is multifactorial. * Clinical heart failure * Asymptomatic ventricular dysfunction * Elevated biomarkers * Severe arrhythmias * Myocardial ischemia * Other cardiac events
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
change in EARLY DETECTION OF CARDIOTOXICITY
Early recognition of cardiotoxicity can help determine whether to continue treatment with a particular type of drug and set up preventive treatments. * Demographic variables for study inclusion * Clinical symptoms of cardiac disease * EKG * Transthoracic echocardiogram * Biological markers: Troponin I (cTnI), NTproBNP * Oncological variables: Diagnosis and cancer location, Drugs
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
Incidence of cardiovascular toxicity in its different forms
Cardiotoxicity severity: * Mild: asymptomatic, no hospitalization needed * Severe: requires admission or specific treatment initiated for this reason
Time frame: 2 years
Incidence of cardiovascular toxicity in relation to the cumulative dose
* Heart failure * Asymptomatic ventricular dysfunction * Myocardial Ischemia * Severe arrhythmias * Other cardiac pathology
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
•Incidence of cardiovascular toxicity in relation to the kind of antitumor agent
* Heart failure * Asymptomatic ventricular dysfunction * Myocardial Ischemia * Severe arrhythmias * Other cardiac pathology
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
•Analyze the sensitivity and specificity of EKG changes regarding new changes in biomarkers, clinical and echocardiographic parameters
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\- EKG
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
Analyze whether alterations of biological markers predate clinical, echocardiographic and functional parameters
* Troponin I * NT-proBNP
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
Compare the effectiveness of early identification of cardiovascular toxicity of high-sensitivity troponin (troponin T) compared to a conventional troponin
* Troponin I (cTn I) * Troponin Thigh sensitivity (cTnhs)
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
Define the sensitivity and specificity of the left ventricle ejection fraction in the detection of cardiovascular toxicity
* Telediastolic volume left ventricle * Telesystolic volume right ventricle * Ejection fraction left ventricle * Size of left atrium * Size right atrium * Mitral valve disease * Tricuspid valve disease * Pericardial overflow
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
• Define the sensitivity and specificity of new ventricular function parameters in cardiovascular toxicity screening.
\- Longitudinal global strain
Time frame: 21 days, 3 months, 6 months, 1 year, 1.5 years and 2 years
Economic analysis derived from the diagnostic strategy with biomarkers versus echocardiography.
Economic analysis comparing efficacy of biomarkers versus echocardiography
Time frame: 2 years