4.7 Article

MicroRNA-4732-3p Is Dysregulated in Breast Cancer Patients with Cardiotoxicity, and Its Therapeutic Delivery Protects the Heart from Doxorubicin-Induced Oxidative Stress in Rats

ANTIOXIDANTS (2022)

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Journal

ANTIOXIDANTS
Volume 11, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/antiox11101955

Keywords

cardiotoxicity; doxorubicin; miR-4732-3p; oxidative stress; fibrosis; angiogenesis; cardiac function; TGF beta pathway; Hippo signaling pathway

Categories

Biochemistry & Molecular Biology Chemistry, Medicinal Food Science & Technology

Funding

  1. Instituto de Salud Carlos III [PI19/0245, RD16/0011/0004, RD16/0011/0037]
  2. FEDER una manera de hacer Europa
  3. INNCON-2020-6-CARVEMO from Agencia Valenciana de Innovacion
  4. Conselleria de Sanitat Universal i Salut Publica [ACIF/2017/318, ACIF/2018/254, ACIF2019/257, ACIF2019/250]
  5. European Union through the Operational Program of the European Regional Development Fund (FEDER) of the Valencian Community 2014-2020

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This study investigated the clinical data of breast cancer patients receiving anthracycline chemotherapy and found that miR-4732-3p is a novel biomarker of cardiotoxicity and may have therapeutic potential against anthracycline-induced heart damage.
Anthracycline-induced cardiotoxicity is the most severe collateral effect of chemotherapy originated by an excess of oxidative stress in cardiomyocytes that leads to cardiac dysfunction. We assessed clinical data from patients with breast cancer receiving anthracyclines and searched for discriminating microRNAs between patients that developed cardiotoxicity (cases) and those that did not (controls), using RNA sequencing and regression analysis. Serum levels of 25 microRNAs were differentially expressed in cases versus controls within the first year after anthracycline treatment, as assessed by three different regression models (elastic net, Robinson and Smyth exact negative binomial test and random forest). MiR-4732-3p was the only microRNA identified in all regression models and was downregulated in patients that experienced cardiotoxicity. MiR-4732-3p was also present in neonatal rat cardiomyocytes and cardiac fibroblasts and was modulated by anthracycline treatment. A miR-4732-3p mimic was cardioprotective in cardiac and fibroblast cultures, following doxorubicin challenge, in terms of cell viability and ROS levels. Notably, administration of the miR-4732-3p mimic in doxorubicin-treated rats preserved cardiac function, normalized weight loss, induced angiogenesis, and decreased apoptosis, interstitial fibrosis and cardiac myofibroblasts. At the molecular level, miR-4732-3p regulated genes of TGF beta and Hippo signaling pathways. Overall, the results indicate that miR-4732-3p is a novel biomarker of cardiotoxicity that has therapeutic potential against anthracycline-induced heart damage.

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