CHANGES IN MYOCARDIAL BIOELECTRIC ACTIVITY IN PATIENTS WITH PROGRESSIVE MYLTIPLE MYELOMA

Abstract

Introduction. Long-termed oncohematological course with periods of progression and remission of multiple myeloma, an increase in the cumulative dose of cytostatic drugs usually lead to a growing risk of chemotherapy-induced cardiotoxicity in patients with high cardiac risks. The aim of this study is to investigate changes in myocardial bioelectric activity of patients with progression of multiple myeloma and concomitant ischemic heart disease. Materials and methods. 42 patients with multiple myeloma were examined. The patients were divided into groups according to presence of concomitant coronary heart disease: І (n=15) included patients with multiple myeloma without concomitant cardiovascular diseases; II (n=27) involved patients with multiple myeloma and concomitant coronary heart disease. The patients were assessed before chemotherapy. We analyzed general and biochemical blood count findings. Based on Holter electrocardiography monitoring findings, we assessed heart rate, PQ interval, corrected QT interval. Results: Grade 3 and 4 of anaemia were detected only in the group of patients with multiple myeloma and concomitant coronary heart disease, in 4 (14,80%) and in 1 (3,70%) patients, respectively. Serum creatinine level above 177 μmol / l was found in 1 (6%) patient in the group I and in 2 (7%) patients in the group II. An inverse correlation was found between creatinine levels and erythrocyte counts in patients with multiple myeloma and concomitant coronary heart disease (R=-0,58, p<0,05). Rhythm disorders were found in 3 (20%) patients with multiple myeloma without cardiovascular diseases and in 8 (29.6%) patients with multiple myeloma with concomitant ischemic heart disease, conduction disorders was found in 5 (33%) patients in group I and in 14 (52%) patients in group II. Tendency in increasing the incidence of myocardial bioelectrical activity has been found out in case of concomitant coronary heart disease.