Cancers (Jun 2022)

A Fibrosis Biomarker Early Predicts Cardiotoxicity Due to Anthracycline-Based Breast Cancer Chemotherapy

  • Ana de la Fuente,
  • Marta Santisteban,
  • Josep Lupón,
  • José Manuel Aramendía,
  • Agnes Díaz,
  • Ana Santaballa,
  • Amparo Hernándiz,
  • Pilar Sepúlveda,
  • Germán Cediel,
  • Begoña López,
  • José María López Picazo,
  • Manuel M. Mazo,
  • Gregorio Rábago,
  • Juan José Gavira,
  • Ignacio García-Bolao,
  • Javier Díez,
  • Arantxa González,
  • Antoni Bayés-Genís,
  • Susana Ravassa

DOI
https://doi.org/10.3390/cancers14122941
Journal volume & issue
Vol. 14, no. 12
p. 2941

Abstract

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Anthracycline-based cancer chemotherapy (ACC) causes myocardial fibrosis, a lesion contributing to left ventricular dysfunction (LVD). We investigated whether the procollagen-derived type-I C-terminal-propeptide (PICP): (1) associates with subclinical LVD (sLVD) at 3-months after ACC (3m-post-ACC); (2) predicts cardiotoxicity 1-year after ACC (12m-post-ACC) in breast cancer patients (BC-patients); and (3) associates with LVD in ACC-induced heart failure patients (ACC-HF-patients). Echocardiography, serum PICP and biomarkers of cardiomyocyte damage were assessed in two independent cohorts of BC-patients: CUN (n = 87) at baseline, post-ACC, and 3m and 12m (n = 65)-post-ACC; and HULAFE (n = 70) at baseline, 3m and 12m-post-ACC. Thirty-seven ACC-HF-patients were also studied. Global longitudinal strain (GLS)-based sLVD (3m-post-ACC) and LV ejection fraction (LVEF)-based cardiotoxicity (12m-post-ACC) were defined according to guidelines. BC-patients: all biomarkers increased at 3m-post-ACC versus baseline. PICP was particularly increased in patients with sLVD (interaction-p p p ≤ 0.025) in both BC-cohorts, adding prognostic value to the early assessment of GLS and LVEF. ACC-HF-patients: PICP was inversely associated with LVEF (p = 0.004). In ACC-treated BC-patients, an early increase in PICP is associated with early sLVD and predicts cardiotoxicity 1 year after ACC. PICP is also associated with LVD in ACC-HF-patients.

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