Hippocampal Adult Neurogenesis Is Maintained by Neil3-Dependent Repair of Oxidative DNA Lesions in Neural Progenitor Cells

Regnell, Christine Elisabeth; Hildrestrand, Gunn A.; Sejersted, Yngve; Medin, Tirill; Moldestad, Olve; Rolseth, Veslemøy; Krokeide, Silje Zandstra; Suganthan, Rajikala; Luna, Luisa; Bjørås, Magnar; Bergersen, Linda H

doi:10.1016/j.celrep.2012.08.008

Cited by 90 publications

(94 citation statements)

References 43 publications

(54 reference statements)

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“…At the cellular level, loss of BER of oxidative lesions is associated with in impaired proliferation of neurospheres from Polb À/À and Neil3 À/À mice (Sugo et al, 2000;Regnell et al, 2012). In our experiments, NSPC cultures derived from hMTH1-Tg mice proliferated better than those from wild-type animals, suggesting that enhanced protection against oxidative damage provides a proliferative advantage.…”

Section: Discussionmentioning

confidence: 47%

“…hMTH1 overexpression increases the proliferative capacity of adult neural stem/progenitor cells As BER-defective mice (Polb À/À and Neil3 À/À mice) may show altered neurogenesis (Sugo et al, 2000;Regnell et al, 2012), we investigated whether hMTH1 overexpression provided some neurogenic advantage. To this end, we assessed the formation of neurospheres generated by adult neural stem/progenitor cells…”

Section: Increased Hmth1 Expression Enhances Exploration Of Environmementioning

confidence: 99%

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Prolonged lifespan with enhanced exploratory behavior in mice overexpressing the oxidized nucleoside triphosphatase hMTH1

et al. 2013

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SummaryThe contribution that oxidative damage to DNA and/or RNA makes to the aging process remains undefined. In this study, we used the hMTH1-Tg mouse model to investigate how oxidative damage to nucleic acids affects aging. hMTH1-Tg mice express high levels of the hMTH1 hydrolase that degrades 8-oxodGTP and 8-oxoGTP and excludes 8-oxoguanine from both DNA and RNA. Compared to wild-type animals, hMTH1-overexpressing mice have significantly lower steady-state levels of 8-oxoguanine in both nuclear and mitochondrial DNA of several organs, including the brain. hMTH1 overexpression prevents the age-dependent accumulation of DNA 8-oxoguanine that occurs in wild-type mice. These lower levels of oxidized guanines are associated with increased longevity and hMTH1-Tg animals live significantly longer than their wild-type littermates. Neither lipid oxidation nor overall antioxidant status is significantly affected by hMTH1 overexpression. At the cellular level, neurospheres derived from adult hMTH1-Tg neural progenitor cells display increased proliferative capacity and primary fibroblasts from hMTH1-Tg embryos do not undergo overt senescence in vitro. The significantly lower levels of oxidized DNA/RNA in transgenic animals are associated with behavioral changes. These mice show reduced anxiety and enhanced investigation of environmental and social cues. Longevity conferred by overexpression of a single nucleotide hydrolase in hMTH1-Tg animals is an example of lifespan extension associated with healthy aging. It provides a link between aging and oxidative damage to nucleic acids.

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Section: Discussionmentioning

confidence: 47%

Section: Increased Hmth1 Expression Enhances Exploration Of Environmementioning

confidence: 99%

Prolonged lifespan with enhanced exploratory behavior in mice overexpressing the oxidized nucleoside triphosphatase hMTH1

et al. 2013

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“…[29,30] NEIL3-null mice showed learning and memory deficits and reduced anxiety-like behavior, and synaptic irregularities in hippocampal neurons. [31] All together, these results suggest that NEIL3 may have a specific role in neurogenesis in the central nervous system. The NEIL3 has been shown to be highly expressed in many tumor tissues, which supports the notion that NEIL3 might be associated with proliferation capacity.…”

Section: Neil3 Expression Patternsmentioning

confidence: 78%

“…NEIL3-null mice also showed learning and memory deficits and reduced anxiety-like behavior, and synaptic irregularities in hippocampal neurons. [31] Future studies addressing the role of NEIL3 in neuronal tissue in ischemic stroke will shed more light on this issue.…”

Section: Neil3mentioning

confidence: 99%

The endonuclease VIII-like proteins: new targets in the treatment of ischemic stroke?

Yang¹,

Wang²,

Zhang³

et al. 2015

Neuroimmunol Neuroinflammation

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Oxidative deoxyribonucleic acid (DNA) damage is one of the major causes of neuronal injury in ischemia. The endonuclease VIII-like (NEIL) DNA glycosylases have a specific role in recognition and removal of oxidative DNA damage. The NEIL family includes NEIL1, NEIL2, and NEIL3, that differ in substrate specificity, catalytic efficiency, and subcellular/tissue distribution. This opens for a situation-dependent phenotype in their absence. In this review, we will discuss the current knowledge on the involvement of the NEILs in ischemic stroke and discuss the potential of these enzymes to serve as new targets in the treatment of ischemic stroke. Received: 24-04-2015; Accepted: 21-08-2015 This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 3.0 License, which allows others to remix, tweak, and build upon the work non-commercially, as long as the author is credited and the new creations are licensed under the identical terms.

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“…In mice, Neil3 is found to be highly expressed in hematopoietic tissue and testis, during embryonic development and in progenitor rich regions in the brain, while human NEIL3 is found to be highly expressed in thymus, testis and in multiple forms of cancer [28][29][30][31][32]. Recently, we showed that murine Neil3 is important for maintenance of cognitive performance [33] and regeneration of neural tissue after perinatal hypoxia-ischemia [32], indicating a role of Neil3 in neurogenesis and protection against hypoxiainduced tissue damage. Thus, several studies indicate a role for NEIL3/Neil3 during cell proliferation, and it is therefore not clear whether canonical repair of oxidative DNA base lesions is the only function of NEIL3.…”

Section: Discussionmentioning

confidence: 97%

Genetic variants in the DNA repair gene NEIL3 and the risk of myocardial infarction in a nested case–control study. The HUNT Study

et al. 2015

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Hippocampal Adult Neurogenesis Is Maintained by Neil3-Dependent Repair of Oxidative DNA Lesions in Neural Progenitor Cells

Cited by 90 publications

References 43 publications

Prolonged lifespan with enhanced exploratory behavior in mice overexpressing the oxidized nucleoside triphosphatase hMTH1

Prolonged lifespan with enhanced exploratory behavior in mice overexpressing the oxidized nucleoside triphosphatase hMTH1

The endonuclease VIII-like proteins: new targets in the treatment of ischemic stroke?

Genetic variants in the DNA repair gene NEIL3 and the risk of myocardial infarction in a nested case–control study. The HUNT Study

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