Lack of the Antioxidant Glutathione Peroxidase-1 (GPx1) Exacerbates Retinopathy of Prematurity in Mice

Tan, Sihmin; Stefanovic, Nada; Tan, Genevieve; Wilkinson-Berka, Jennifer L.; Haan, Judy B. de

doi:10.1167/iovs.12-10685

Cited by 42 publications

(33 citation statements)

References 44 publications

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“…GPx3 is an intracellular enzyme actively released into the plasma so the significance of its elevation in the σ1RKO neural retina is not clear, nor its elevation in the present study of Müller cells. Most studies of glutathione peroxidase in retina have focused on GPx1 [48,49], therefore in our studies we investigated its expression in σ1RKO Müller cells and found a significant decrease at the gene and protein level. In our investigation of Gpx2 gene expression; we observed no significant difference between σ1RKO Müller cells versus WT.…”

Section: Discussionmentioning

confidence: 97%

Sigma 1 receptor regulates the oxidative stress response in primary retinal Müller glial cells via NRF2 signaling and system xc−, the Na+-independent glutamate–cystine exchanger

Wang

Shanmugam

Markand

et al. 2015

Free Radical Biology and Medicine

114

112

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Oxidative stress figures prominently in retinal diseases including diabetic retinopathy and glaucoma. Ligands for σ1R, a unique transmembrane protein localized to the ER, mitochondria, nuclear and plasma membrane, have profound retinal neuroprotective properties in vitro and in vivo. Studies to determine the mechanism of σ1R-mediated retinal neuroprotection have focused mainly on neurons. Little is known about effects of σ1R on Müller cell function, yet these radial glial cells are essential for homeostatic support of the retina. Here we investigated whether σ1R mediates the oxidative stress response of Müller cells using wildtype (WT) and σ1R knockout (σ1RKO) mice. We observed increased endogenous ROS levels in σ1RKO Müller cells compared to WT, which was accompanied by decreased expression of Sod1, Catalase, Nqo1, Hmox1, Gstm6 and Gpx1. The protein levels of SOD1, CAT, NQO1 and GPX1 were also significantly decreased. The genes encoding these antioxidants contain an antioxidant response element (ARE), which under stress is activated by NRF2, a transcription factor that typically resides in the cytoplasm bound by KEAP1. In the σ1RKO Müller cells Nrf2 expression was decreased significantly at the gene (and protein) level, while Keap1 gene (and protein) levels were markedly increased. NRF2-ARE binding affinity was decreased markedly in σ1RKO Müller cells. We investigated system xc−, the cystine-glutamate exchanger important for synthesis of GSH, and observed decreased function in σ1RKO Müller cells compared to WT as well as decreased GSH and GSH/GSSG ratios. This was accompanied by decreased gene and protein levels of xCT, the unique component of system xc−. We conclude that Müller glial cells lacking σ1R manifest elevated ROS, perturbation of antioxidant balance, suppression of NRF2 signaling and impaired function of system xc−. The data suggest that the oxidative stress-mediating function of retinal Müller glial cells may be compromised in the absence of σ1R. The neuroprotective role of σ1R may be linked directly to the oxidative stress-mediating properties of supportive glial cells.

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Section: Discussionmentioning

confidence: 97%

Sigma 1 receptor regulates the oxidative stress response in primary retinal Müller glial cells via NRF2 signaling and system xc−, the Na+-independent glutamate–cystine exchanger

Wang

Shanmugam

Markand

et al. 2015

Free Radical Biology and Medicine

114

112

View full text Add to dashboard Cite

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“…Recent studies have shown a pivotal role for the ubiquitously expressed antioxidant enzyme GPx1 in limiting retinal injury 94. Using the OIR model, studies showed that lack of GPx1 led to increased ROS production, significant vaso‐obliteration of the retinal vasculature and intravitreous neovascularisation.…”

Section: Diabetic Retinopathy Antioxidant Defences and Immunotherapiesmentioning

confidence: 99%

“…Recent studies have shown a pivotal role for the ubiquitously expressed antioxidant enzyme GPx1 in limiting retinal injury. 94 Using the OIR model, studies showed that lack of GPx1 led to increased ROS production, significant vaso-obliteration of the retinal vasculature and intravitreous neovascularisation. At the molecular level, lack of GPx1 caused significant increase in VEGF that was most likely responsible for the modest yet significant, neovascularisation observed in this model.…”

Section: Targeting Oxidative Stress In Diabetic Retinopathymentioning

confidence: 99%

Recent novel approaches to limit oxidative stress and inflammation in diabetic complications

et al. 2018

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Diabetes is considered a major burden on the healthcare system of Western and non‐Western societies with the disease reaching epidemic proportions globally. Diabetic patients are highly susceptible to developing micro‐ and macrovascular complications, which contribute significantly to morbidity and mortality rates. Over the past decade, a plethora of research has demonstrated that oxidative stress and inflammation are intricately linked and significant drivers of these diabetic complications. Thus, the focus now has been towards specific mechanism‐based strategies that can target both oxidative stress and inflammatory pathways to improve the outcome of disease burden. This review will focus on the mechanisms that drive these diabetic complications and the feasibility of emerging new therapies to combat oxidative stress and inflammation in the diabetic milieu.

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“…Both hyperoxia and hypoxia can induce ROS generation 45. In the mouse OIR model, mice deficient in glutathione peroxidase, one of the antioxidant enzymes, showed increased ROS generation, VEGF expression, and neovascular area in the retina 63. Reduction of ROS production in aldose reductase-deficient mice reduced vaso-obliteration and neovascular tufts by downregulating VEGF expression in the retina 64.…”

Section: Signaling Pathways Involved In Vegf Expression and Vegf-medimentioning

confidence: 99%

Anti-VEGF therapy in the management of retinopathy of prematurity: what we learn from representative animal models of oxygen-induced retinopathy

Wang

2016

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Retinopathy of prematurity (ROP) remains a leading cause of childhood blindness, affecting infants born prematurely. ROP is characterized by the onset of delayed physiological retinal vascular development (PRVD) and followed by pathologic neovascularization into the vitreous instead of the retina, called intravitreal neovascularization (IVNV). Therefore, the therapeutic strategy for treating ROP is to promote PRVD and inhibit or prevent IVNV. Vascular endothelial growth factor (VEGF) plays an important role in the pathogenesis of ROP. There is a growing body of studies testing the use of anti-VEGF agents as a treatment for ROP. Intravitreal anti-VEGF treatment for ROP has potential advantages compared with laser photocoagulation, the gold standard for the treatment of severe ROP; however, intravitreal anti-VEGF treatment has been associated with reactivation of ROP and suppression of systemic VEGF that may affect body growth and organ development in preterm infants. Therefore, it is important to understand the role of VEGF in PRVD and IVNV. This review includes the current knowledge of anti-VEGF treatment for ROP from animal models of oxygen-induced retinopathy (OIR), highlighting the importance of VEGF inhibition by targeting retinal Müller cells, which inhibits IVNV and permits PRVD. The signaling events involved in mediating VEGF expression and promoting VEGF-mediated angiogenesis, including hypoxia-dependent signaling, erythropoietin/erythropoietin receptor-, oxidative stress-, beta-adrenergic receptor-, integrin-, Notch/Delta-like ligand 4- and exon guidance molecules-mediated signaling pathways, are also discussed.

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Lack of the Antioxidant Glutathione Peroxidase-1 (GPx1) Exacerbates Retinopathy of Prematurity in Mice

Cited by 42 publications

References 44 publications

Sigma 1 receptor regulates the oxidative stress response in primary retinal Müller glial cells via NRF2 signaling and system xc−, the Na+-independent glutamate–cystine exchanger

Sigma 1 receptor regulates the oxidative stress response in primary retinal Müller glial cells via NRF2 signaling and system xc−, the Na+-independent glutamate–cystine exchanger

Recent novel approaches to limit oxidative stress and inflammation in diabetic complications

Anti-VEGF therapy in the management of retinopathy of prematurity: what we learn from representative animal models of oxygen-induced retinopathy

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