Paradoxical role of the NADPH oxidase NOX4 in early preneoplastic stages of hepatocytes induced by amino acid deprivation

• Published in: Biochimica et biophysica acta. General subjects Vol. 1863; no. 4; pp. 714 - 722
• Main Authors: Campisano, Sabrina, Bertran, Esther, Caballero-Díaz, Daniel, La Colla, Anabela, Fabregat, Isabel, Chisari, Andrea Nancy
• Format: Journal Article
• Language: English
• Published: Netherlands Elsevier B.V 01.04.2019
• Subjects: Amino acid deprivation; amino acids; antioxidants; biomarkers; caspase-3; cell proliferation; Epidermal growth factor receptor; epidermal growth factor receptors; hepatocytes; hepatoma; molecular biology; NAD(P)H oxidase (H2O2-forming); NADPH oxidase 4; phenotype; Reactive oxygen species; signal transduction; therapeutics; transforming growth factor beta; Transforming growth factor β; Aa; Par; NAFLD; Reactive oxygen species; Amino acid deprivation; PI-3K; Transforming growth factor β; HCC; H2DCFDA; γ-GCS; MAPK; EGFR; Epidermal growth factor receptor; ERKs; NOX; FBS; ROS; TGF-β; NADPH oxidase 4; Sel; PM; GSH; Transforming Growth factor β; Reactive Oxygen Species; Epidermal Growth factor Receptor
• ISSN: 0304-4165; 1872-8006; 1872-8006
• DOI: 10.1016/j.bbagen.2019.01.017

The NADPH oxidase (NOX) 4 is an important source of ROS in signal transduction that acts as a liver tumor suppressor. Transforming Growth Factor β (TGF-β) and Epidermal Growth Factor Receptor (EGFR) pathways are involved in the modulation of NOX4 expression. Data showed that recurrent protein deprivation induces changes distinctive of a preneoplastic profile. However, the mechanisms underneath these changes have not been completely understood. Hepatocytes that survived to the lack of amino acids (Aa) (Sel line) were cultured in complete or Aa free medium. We elucidated the molecular mechanisms that support such preneoplastic alterations employing biochemical and molecular biology assays. Sel line showed increased phospho-AKT and phospho-ERKs levels, diminished caspase-3 activity, augmented cell proliferation and overactivation of EGFR pathway, reminiscent of a preneoplastic phenotype. NOX4 was upregulated in these cells by TGF-β canonical pathway, however ROS levels were not found increased as a result of an increment of antioxidant enzymes. Inhibition of TGF-β receptor diminished NOX4 and strikingly, after EGFR inhibition, NOX4 levels also decreased. Therefore, both TGF-β and EGFR pathways are shown to be involved in the upregulation of NOX4 in Sel line. This work provides novel results regarding to the regulation of NOX4 in the preneoplastic transformation of hepatocytes in the absence of Aa, in the context of TGF-β and EGFR pathways. The advances in the understanding of the molecular mechanisms whose deregulation ultimately causes Hepatocellular Carcinoma (HCC) are essential to prevent it and to design diagnostic biomarkers and therapeutic tools. •Hepatocytes that survived to lack of amino acids act as a preneoplastic cell line.•NOX4 increases in hepatocytes cultured under amino acid deprivation.•Lack of amino acids increments catalase and γ-GSC levels in hepatocytes.•EGFR and TGF-β pathways are involved in NOX4 increase in preneoplastic hepatocytes.•EGFR and TGF-β pathways can transactivate each other in preneoplastic hepatocytes.