Redox and metal profiles in human coronary endothelial and smooth muscle cells under hyperoxia, physiological normoxia and hypoxia: Effects of NRF2 signaling on intracellular zinc

Matthew J Smith; Fan Yang; Alexander Griffiths; Alexander Morrell; Sarah J Chapple; Richard C M Siow; Theodora Stewart; Wolfgang Maret; Giovanni E Mann

doi:10.1016/j.redox.2023.102712

Redox and metal profiles in human coronary endothelial and smooth muscle cells under hyperoxia, physiological normoxia and hypoxia: Effects of NRF2 signaling on intracellular zinc

Redox Biol. 2023 Jun:62:102712. doi: 10.1016/j.redox.2023.102712. Epub 2023 Apr 23.

Authors

Matthew J Smith¹, Fan Yang¹, Alexander Griffiths², Alexander Morrell², Sarah J Chapple¹, Richard C M Siow¹, Theodora Stewart³, Wolfgang Maret⁴, Giovanni E Mann⁵

Affiliations

¹ King's British Heart Foundation Centre of Research Excellence, School of Cardiovascular and Metabolic Medicine & Sciences, Faculty of Life Sciences & Medicine, King's College London, 150 Stamford Street, London, SE1 9NH, UK.
² London Metallomics Facility, Faculty of Life Sciences & Medicine, King's College London, UK.
³ Research Management & Innovation Directorate (RMID), King's College London, UK.
⁴ Departments of Biochemistry and Nutritional Sciences, School of Life Course & Population Sciences, Faculty of Life Sciences & Medicine, King's College London, UK.
⁵ King's British Heart Foundation Centre of Research Excellence, School of Cardiovascular and Metabolic Medicine & Sciences, Faculty of Life Sciences & Medicine, King's College London, 150 Stamford Street, London, SE1 9NH, UK. Electronic address: giovanni.mann@kcl.ac.uk.

Abstract

Zinc is an important component of cellular antioxidant defenses and dysregulation of zinc homeostasis is a risk factor for coronary heart disease and ischemia/reperfusion injury. Intracellular homeostasis of metals, such as zinc, iron and calcium are interrelated with cellular responses to oxidative stress. Most cells experience significantly lower oxygen levels in vivo (2-10 kPa O₂) compared to standard in vitro cell culture (18kPa O₂). We report the first evidence that total intracellular zinc content decreases significantly in human coronary artery endothelial cells (HCAEC), but not in human coronary artery smooth muscle cells (HCASMC), after lowering of O₂ levels from hyperoxia (18 kPa O₂) to physiological normoxia (5 kPa O₂) and hypoxia (1 kPa O₂). This was paralleled by O₂-dependent differences in redox phenotype based on measurements of glutathione, ATP and NRF2-targeted protein expression in HCAEC and HCASMC. NRF2-induced NQO1 expression was attenuated in both HCAEC and HCASMC under 5 kPa O₂ compared to 18 kPa O₂. Expression of the zinc efflux transporter ZnT1 increased in HCAEC under 5 kPa O₂, whilst expression of the zinc-binding protein metallothionine (MT) decreased as O₂ levels were lowered from 18 to 1 kPa O₂. Negligible changes in ZnT1 and MT expression were observed in HCASMC. Silencing NRF2 transcription reduced total intracellular zinc under 18 kPa O₂ in HCAEC with negligible changes in HCASMC, whilst NRF2 activation or overexpression increased zinc content in HCAEC, but not HCASMC, under 5 kPa O₂. This study has identified cell type specific changes in the redox phenotype and metal profile in human coronary artery cells under physiological O₂ levels. Our findings provide novel insights into the effect of NRF2 signaling on Zn content and may inform targeted therapies for cardiovascular diseases.

Keywords: Coronary artery endothelial cells; Coronary artery smooth muscle cells; HIF-1α; HO-1; Human coronary artery; Hyperoxia; Hypoxia; ICP-MS; LA-ICP-MS; Metallomics; Metallothionein; Metals; NQO1; NRF2; Oxygen; Physiological normoxia; Redox status; Zn; ZnT1.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Endothelial Cells* / metabolism
Humans
Hyperoxia* / metabolism
Hypoxia / metabolism
Myocytes, Smooth Muscle / metabolism
NF-E2-Related Factor 2 / genetics
NF-E2-Related Factor 2 / metabolism
Oxidation-Reduction
Oxygen / metabolism
Zinc / metabolism

Substances

NF-E2-Related Factor 2
Oxygen
Zinc
NFE2L2 protein, human