Valproic acid promotes SOD2 acetylation: a potential mechanism of valproic acid-induced oxidative stress in developing systems

Jason M Hansen; S Marc Lucas; Catania D Ramos; Eli J Green; Dakota J Nuttall; David S Clark; Erik D Marchant; Chad R Hancock; Ted B Piorczynski

doi:10.1080/10715762.2021.2017913

Valproic acid promotes SOD2 acetylation: a potential mechanism of valproic acid-induced oxidative stress in developing systems

Free Radic Res. 2021 Dec;55(11-12):1130-1144. doi: 10.1080/10715762.2021.2017913. Epub 2022 Jan 19.

Authors

Jason M Hansen¹, S Marc Lucas¹, Catania D Ramos¹, Eli J Green¹, Dakota J Nuttall¹, David S Clark¹, Erik D Marchant², Chad R Hancock², Ted B Piorczynski¹

Affiliations

¹ Department of Cell Biology and Physiology, Brigham Young University, Provo, UT, USA.
² Department of Nutrition, Dietetics and Food Science, College of Life Sciences, Brigham Young University, Provo, UT, USA.

PMID: 34895005
DOI: 10.1080/10715762.2021.2017913

Abstract

Valproic acid (VPA) is an antiepileptic, bipolar, and migraine medication, which is associated with embryonic dysmorphology, more specifically neural tube defects (NTDs), if taken while pregnant. One mechanism by which VPA may cause NTDs is through oxidative stress that cause disruption of cell signaling. However, mechanisms of VPA-induced oxidative stress are not fully understood. Since VPA is a deacetylase inhibitor, we propose that VPA promotes mitochondrial superoxide dismutase-2 (SOD2) acetylation, decreasing SOD2 activity and increasing oxidant levels. Using the pluripotent embryonal carcinoma cell line, P19, VPA effects were evaluated in undifferentiated and neurodifferentiated cells. VPA treatments increased oxidant levels, oxidized the glutathione (GSH)/glutathione disulfide (GSSG) redox couple, and decreased total SOD and SOD2 activity in undifferentiated P19 cells but not in differentiated P19 cells. VPA caused a specific increase in mitochondrial oxidants in undifferentiated P19 cells, VPA did not alter respirometry measurements. Immunoblot analyses demonstrated that VPA increased acetylation of SOD2 at lysine⁶⁸ (AcK68 SOD2) in undifferentiated P19 cells but not in differentiated P19 cells. Pretreatments with the Nrf2 inducer, dithiol-3-thione (D3T), in undifferentiated P19 cells prevented increased oxidant levels, GSH/GSSG redox oxidation and restored total SOD and SOD2 activity, correlating with a decrease in AcK68 SOD2 levels. In embryos, VPA decreased total SOD and SOD2 activity and increased levels of AcK68 SOD2, and D3T pretreatments prevented VPA effects, increasing total SOD and SOD2 activity and lowering levels of AcK68 SOD2. These data demonstrate a potential, contributing oxidizing mechanism by which VPA incites teratogenesis in developing systems. Moreover, these data also suggest that Nrf2 interventions may serve as a means to protect developmental signaling and inhibit VPA-induced malformations.

Keywords: Oxidative stress; acetylation; mitochondria; neural tube defect; superoxide dismutase; valproic acid.

MeSH terms

Acetylation
Antioxidants / metabolism
Female
Glutathione / metabolism
Glutathione Disulfide / metabolism
Humans
NF-E2-Related Factor 2 / metabolism
Neural Tube Defects* / chemically induced
Neural Tube Defects* / metabolism
Oxidants
Oxidative Stress
Pregnancy
Superoxide Dismutase / metabolism
Valproic Acid* / adverse effects

Substances

Antioxidants
NF-E2-Related Factor 2
Oxidants
Valproic Acid
Superoxide Dismutase
superoxide dismutase 2
Glutathione
Glutathione Disulfide