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  Česky / Czech version Klin. Biochem. Metab., 13 (34), 2005, No. 2, p. 107–111.
 
Monitoring of Cardiotoxicity during Induction Chemotherapy in Acute Leukemia with Biochemical Markers 
Horáček J. M.1, 4, Pudil R.2, Tichý M.3, 4, Jebavý L.1, 4 

1II. interní klinika, Oddělení klinické hematologie, Lékařské fakulty Univerzity Karlovy a Fakultní nemocnice Hradec Králové 2 I. interní klinika, Lékařské fakulty Univerzity Karlovy a Fakultní nemocnice Hradec Králové 3 Ústav klinické biochemie a diagnostiky, Lékařské fakulty Univerzity Karlovy a Fakultní nemocnice Hradec Králové 4 Katedra válečného vnitřního lékařství, Fakulta vojenského zdravotnictví Univerzity obrany Hradec Králové
 


Summary:

       Introduction: Cardiotoxicity is a well-known and serious complication of antitumorous treatment. Anthracyclines represent the greatest risk. Biochemical markers of structural and functional myocardial damage have been gaining ground in cardiotoxicity diagnostics. Design: Monitoring of cardiotoxicity during induction chemotherapy in acute myeloid leukemia (AML) patients and assessment of potential for use of biochemical markers in early diagnostics of cardiotoxicity. Patients and Methods: 15 consecutive adult patients with a newly diagnosed AML (9 male and 6 female, mean age 43.7 ± 10.6 years) participated in the study. The patients received induction chemotherapy containing intermediate doses of Cytarabine (8 x 1.5 g/m2) and Idarubicin (IDA) 12 mg/m2/day intravenously on 1st 3rd and 5th day (in total 36 mg/m2 = 1/4 of the maximum cumulative dose). Serial measurements of serum NT-proBNP concentrations were performed at the baseline, the day following each IDA infusion, after 14 days and after circa 1 month, i.e. before the next chemotherapy. Cardiospecific markers (cTnT, CK-MB mass) were measured at the baseline and after the last IDA infusion. Results: The mean baseline concentration of NT-proBNP in newly diagnosed AML patients was 129.7 ± 59.6 pg/ml. The mean value of the NT-proBNP concentration increased after the first IDA infusion to 307.3 ± 171.4 pg/ml (P = 0.02). In most of the patients the second and the third IDA infusions were not associated with a further increase in the NT-proBNP value and values after 2 or 4 weeks were not significantly different from the baseline. However, in one of the patients the NT- -proBNP values were increasing after each IDA infusion (after the last one 786.2 pg/ml) and within 14 days he developed congestive heart failure due to left ventricular diastolic dysfunction as assessed by echocardiography. At that time the NTproBNP value was 1184.0 pg/ml; after diuretics it decreased significantly. In all patients plasma cTnT and CK-MB mass concentrations were within the reference interval at the baseline and after the induction chemotherapy. Conclusions: Our results show that induction chemotherapy in AML (IDA 36 mg/m2 and intermediate doses of Cytarabine): 1. does not cause detectable damage of the myocyte structure; 2. is in all patients associated with acute neurohumoral activation (transient elevation of NT-proBNP) indicating acute subclinical cardiotoxicity, 3. may lead to congestive heart failure and NT-proBNP seems to be a promising early marker and predictor of this complication.

        Key words: NT-proBNP, cardiomarkers, cardiotoxicity, anthracyclines, acute leukemia.
       

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