Grant Details
| Grant Number: | 1R21CA178344-01 Interpret this number |
| Primary Investigator: | Armenian, Saro |
| Organization: | Beckman Research Institute/City Of Hope |
| Project Title: | Anthraycline-Related Cardiotoxicity in Long-Term Survivors of Lymphoma |
| Fiscal Year: | 2013 |
Abstract
DESCRIPTION (provided by applicant): Anthracyclines form the backbone of therapy for lymphoma (Hodgkin [HL] and non-Hodgkin lymphoma [NHL]). However, the use of anthracyclines is limited by a dose-dependent association between anthracyclines and risk of cardiotoxicity that can lead to congestive heart failure (CHF). Lymphoma survivors are at a 2- to 5-fold increased risk of developing CHF when compared with the general population; autologous hematopoietic cell transplantation (HCT) survivors have an especially high risk. The overall prognosis is poor - five-year survival is less than 50% after CHF diagnosis. Anthracycline-induced CHF is a progressive disorder, with a period of asymptomatic left ventricular (LV) dysfunction characterized by dilation of the LV chamber, thinning of the myocardial wall, and increase in LV end-systolic wall stress (ESWS), a well-established precursor that precedes other indices of systolic function (LV ejection fraction [EF] and shortening fraction [SF]). Traditionally, detection of anthracycline-related LV dysfunction has relied upon echocardiographic screening using resting EF and SF. However, these parameters represent late-occurring changes in myocardial function. By the time decline in EF and SF are detected, functional deterioration is essentially irreversible, emphasizing the need for biomarkers that would facilitate identification of cardiac damage at an earlier stage, such that effective interventions can halt or reverse the process and prevent development of overt CHF. We have recently completed a study describing sensitive echocardiographic indices and blood biomarkers in childhood cancer survivors, and are now conducting a pharmacologic intervention to reverse myocardial remodeling in childhood cancer survivors at high risk for CHF. In the proposed study, we aim to address these gaps in anthracycline- exposed adults with lymphoma. Using a cross-sectional study design, this proposal will examine the role of novel echocardiographic (Tissue Doppler imaging, myocardial deformation [speckle tracking echocardiography], 2D- M-mode derived diastolic and systolic indices) and blood (cardiac troponins, natriuretic peptides, Galectin-3, ST-2, metabolomics) indices in detecting LV dysfunction (abnormal ESWS) in adult lymphoma survivors treated with anthracyclines. We will also measure these indices in age- and sex-matched healthy controls, in order to define the range for non-anthracycline-exposed individuals, and use these values to describe the magnitude of abnormality in the anthracycline-exposed lymphoma survivors. The current study's innovation lies in its ability to leverage existing information from childhood cancer survivors and non- oncology populations to develop a comprehensive assessment of cardiac function in adults with lymphoma. Information obtained from this study may be used to develop more comprehensive screening strategies in at risk populations, and to use these intermediate endpoints for pharmacologic interventions aimed at preventing CHF in survivors with early LV dysfunction.
Publications
Prevalence of anthracycline-related cardiac dysfunction in long-term survivors of adult-onset lymphoma.
Authors: Armenian S.H. , Mertens L. , Slorach C. , Venkataraman K. , Mascarenhas K. , Nathwani N. , Wong F.L. , Forman S.J. , Bhatia S. .
Source: Cancer, 2018-02-15; 124(4), p. 850-857.
EPub date: 2017-11-07.
PMID: 29112235
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Carnitine and cardiac dysfunction in childhood cancer survivors treated with anthracyclines.
Authors: Armenian S.H. , Gelehrter S.K. , Vase T. , Venkatramani R. , Landier W. , Wilson K.D. , Herrera C. , Reichman L. , Menteer J.D. , Mascarenhas L. , et al. .
Source: Cancer epidemiology, biomarkers & prevention : a publication of the American Association for Cancer Research, cosponsored by the American Society of Preventive Oncology, 2014 Jun; 23(6), p. 1109-14.
EPub date: 2014-04-09.
PMID: 24718281
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