Abstract

BackgroundIron overload cardiomyopathy remains the major cause of death in patients with transfusion-dependent thalassemia. Cardiac T2* magnetic resonance imaging is costly yet effective in detecting cardiac iron accumulation in the heart. Heart rate variability (HRV) has been used to evaluate cardiac autonomic function and is depressed in cases of thalassemia. We evaluated whether HRV could be used as an indicator for early identification of cardiac iron deposition.MethodsOne hundred and one patients with transfusion-dependent thalassemia were enrolled in this study. The correlation between recorded HRV and hemoglobin, non-transferrin bound iron (NTBI), serum ferritin and cardiac T2* were evaluated.ResultsThe median age was 18 years (range 8–59 years). The patient group with a 5-year mean serum ferritin >5,000 ng/mL included significantly more homozygous β-thalassemia and splenectomized patients, had lower hemoglobin levels, and had more cardiac iron deposit than all other groups. Anemia strongly influenced all domains of HRV. After adjusting for anemia, neither serum ferritin nor NTBI impacted the HRV. However cardiac T2* was an independent predictor of HRV, even after adjusting for anemia. For receiver operative characteristic (ROC) curve analysis of cardiac T2* ≤20 ms, only mean ferritin in the last 12 months and the average of the standard deviation of all R-R intervals for all five-minute segments in the 24-hour recording were predictors for cardiac T2* ≤20 ms, with area under the ROC curve of 0.961 (p<0.0001) and 0.701 (p = 0.05), respectively.ConclusionsHemoglobin and cardiac T2* as significant predictors for HRV indicate that anemia and cardiac iron deposition result in cardiac autonomic imbalance. The mean ferritin in the last 12 months could be useful as the best indicator for further evaluation of cardiac risk. The ability of serum ferritin to predict cardiac risk is stronger than observed in other thalassemia cohorts. HRV might be a stronger predictor of cardiac iron in study populations with lower somatic iron burdens and greater prevalence of cardiac iron deposition.

Highlights

  • Thalassemia is a hereditary blood disorder caused by a defective synthesis of the globin chains that are the main components of hemoglobin

  • The ability of serum ferritin to predict cardiac risk is stronger than observed in other thalassemia cohorts

  • Heart rate variability (HRV) might be a stronger predictor of cardiac iron in study populations with lower somatic iron burdens and greater prevalence of cardiac iron deposition

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Summary

Introduction

Thalassemia is a hereditary blood disorder caused by a defective synthesis of the globin chains that are the main components of hemoglobin. Transfusion-dependent thalassemia (TDT) is a subset of thalassemia that requires regular red blood cell transfusions for survival. The mainstay of long-term management is red blood cell transfusion. A serious consequence of iron deposition is cardiotoxicity, the leading cause of death among these patients. The survival of TDT patients is determined by the amount of iron accumulation within the heart [3,4]. There are many iron chelators currently available that are effective at removing excess accumulated iron, the mortality of TDT remains high [5,6,7,8,9]. Iron overload cardiomyopathy remains the major cause of death in patients with transfusion-dependent thalassemia. Heart rate variability (HRV) has been used to evaluate cardiac autonomic function and is depressed in cases of thalassemia. We evaluated whether HRV could be used as an indicator for early identification of cardiac iron deposition

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