Potential role of epicardial adipose tissue as a biomarker of anthracycline cardiotoxicity

Potential role of epicardial adipose tissue as a biomarker of anthracycline cardiotoxicity

Abstract Background We investigated the radiodensity of epicardial (EAT), subcutaneous (SAT), and visceral adipose tissue (VAT) before and after treatment with anthracyclines in a population of breast cancer (BC) patients, and in controls not treated with anthracyclines, to detect a potential role o...

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Autores principales: Caterina Beatrice Monti, Simone Schiaffino, Maria Del Mar Galimberti Ortiz, Davide Capra, Moreno Zanardo, Elena De Benedictis, Alberto Gianluigi Luporini, Pietro Spagnolo, Francesco Secchi, Francesco Sardanelli
Formato: article
Lenguaje:EN
Publicado: SpringerOpen 2021
Materias:
Anthracyclines
Cardiotoxicity
Breast neoplasms
Biomarkers
Tomography, X-ray computed
Medical physics. Medical radiology. Nuclear medicine
R895-920
Acceso en línea:https://doaj.org/article/2ca2caf490e54e20b6e7a1b6ae8ada30
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Sumario:Abstract Background We investigated the radiodensity of epicardial (EAT), subcutaneous (SAT), and visceral adipose tissue (VAT) before and after treatment with anthracyclines in a population of breast cancer (BC) patients, and in controls not treated with anthracyclines, to detect a potential role of EAT density as a biomarker of changes related to chemotherapy cardiotoxicity. Methods We reviewed BC patients treated with anthracyclines who underwent CT before (CT-t0) and after (CT-t1) chemotherapy, and age- and sex-matched controls who underwent two CT examinations at comparable intervals. On non-contrast scans, EAT was segmented contouring the pericardium and thresholding between -190 and -30 Hounsfield units (HU), and SAT and VAT were segmented with two 15-mm diameter regions of interest thresholded between -195 and -45 HU. Results Thirty-two female patients and 32 controls were included. There were no differences in age (p = 0.439) and follow-up duration (p = 0.162) between patients and controls. Between CT-t0 and CT-t1, EAT density decreased in BC patients (-66 HU, interquartile range [IQR] -71 to -63 HU, to -71 HU, IQR -75 to -66 HU, p = 0.003), while it did not vary in controls (p = 0.955). SAT density increased from CT-t0 to CT-t1 in BC patients (-107 HU, IQR -111 to -105 HU, to -105 HU, IQR -110 to -100 HU, p = 0.014), whereas it did not change in controls (p = 0.477). VAT density did not vary in either BC patients (p = 0.911) or controls (p = 0.627). Conclusions EAT density appears to be influenced by anthracycline treatment for BC, well known for its cardiotoxicity, shifting towards lower values indicative of a less active metabolism.

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