Literature DB >> 29383682

Disruption of De Novo Serine Synthesis in Müller Cells Induced Mitochondrial Dysfunction and Aggravated Oxidative Damage.

Ting Zhang1,2, Mark C Gillies2, Michele C Madigan2,3, Weiyong Shen2, Jianhai Du4, Ulrike Grünert2, Fanfan Zhou5, Michelle Yam2, Ling Zhu6.   

Abstract

De novo serine synthesis plays important roles in normal mitochondrial function and cellular anti-oxidative capacity. It is reported to be mainly activated in glial cells of the central nervous system, but its role in retinal Müller glia remains unclear. In this study, we inhibited de novo serine synthesis using CBR-5884, a specific inhibitor of phosphoglycerate dehydrogenase (PHGDH, a rate limiting enzyme in de novo serine metabolism) in MIO-M1 cells (immortalized human Müller cells) and huPMCs (human primary Müller cells) under mild oxidative stress. Alamar blue and LDH (lactate dehydrogenase) assays showed significantly reduced metabolic activities and increased cellular damage of Müller cells, when exposed to CBR-5884 accompanied by mild oxidative stress; however, CBR-5884 alone had little effect. The increased cellular damage was partially reversed by supplementation with exogenous serine/glycine. HSP72 (an oxidative stress marker) and reactive oxygen species (ROS) levels were significantly increased; glutathione and NADPH/NADP+ levels were pronouncedly reduced under PHGDH inhibition accompanied by oxidative stress. JC-1 staining and Seahorse respiration experiments showed that inhibition of de novo serine synthesis in Müller cells can also increase mitochondrial stress and decrease mitochondrial ATP production. qPCR and Western blot demonstrated an increased expression of HSP60 (a key mitochondrial stress-related gene), and this was further validated in human retinal explants. Our study suggests that de novo serine synthesis is important for Müller cell survival, particularly when they are exposed to mild oxidative stress, possibly by maintaining mitochondrial function and generating glutathione and NADPH to counteract ROS.

Entities:  

Keywords:  De novo serine synthesis; Glutathione; Mitochondrial dysfunction; Müller cells; Oxidative stress; Phosphoglycerate dehydrogenase

Mesh:

Substances:

Year:  2018        PMID: 29383682     DOI: 10.1007/s12035-017-0840-8

Source DB:  PubMed          Journal:  Mol Neurobiol        ISSN: 0893-7648            Impact factor:   5.590


  36 in total

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7.  Identification of a small molecule inhibitor of 3-phosphoglycerate dehydrogenase to target serine biosynthesis in cancers.

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Review 6.  The unfolded protein response signaling and retinal Müller cell metabolism.

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Journal:  Neural Regen Res       Date:  2018-11       Impact factor: 5.135

7.  Human macular Müller cells rely more on serine biosynthesis to combat oxidative stress than those from the periphery.

Authors:  Ting Zhang; Ling Zhu; Michele C Madigan; Wei Liu; Weiyong Shen; Svetlana Cherepanoff; Fanfan Zhou; Shaoxue Zeng; Jianhai Du; Mark C Gillies
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10.  Weanling Offspring of Dams Maintained on Serine-Deficient Diet Are Vulnerable to Oxidative Stress.

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