Epigenetic aging in adult neurogenesis.

Zocher, Sara; Toda, Tomohisa

doi:10.1002/hipo.23494

Items
Marc 21

001			169366
005			20231120155332.0
024	7	_	\|a 10.1002/hipo.23494 \|2 doi
024	7	_	\|a pmid:36624660 \|2 pmid
024	7	_	\|a 1050-9631 \|2 ISSN
024	7	_	\|a 1098-1063 \|2 ISSN
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037	_	_	\|a DZNE-2023-00141
041	_	_	\|a English
082	_	_	\|a 610
100	1	_	\|a Zocher, Sara \|0 P:(DE-2719)2810548 \|b 0 \|e First author \|u dzne
245	_	_	\|a Epigenetic aging in adult neurogenesis.
260	_	_	\|a New York, NY [u.a.] \|c 2023 \|b Wiley
336	7	_	\|a article \|2 DRIVER
336	7	_	\|a Output Types/Journal article \|2 DataCite
336	7	_	\|a Journal Article \|b journal \|m journal \|0 PUB:(DE-HGF)16 \|s 1680532540_25881 \|2 PUB:(DE-HGF) \|x Review Article
336	7	_	\|a ARTICLE \|2 BibTeX
336	7	_	\|a JOURNAL_ARTICLE \|2 ORCID
336	7	_	\|a Journal Article \|0 0 \|2 EndNote
500	_	_	\|a Funding information: Deutsche Forschungsgemeinschaft, Grant/Award Numbers: TO1347/4-1, TO1347/3-1; H2020 European Research Council, Grant/Award Numbers: EAGER, 804468
520	_	_	\|a Neural stem cells (NSCs) in the hippocampus generate new neurons throughout life, which functionally contribute to cognitive flexibility and mood regulation. Yet adult hippocampal neurogenesis substantially declines with age and age-related impairments in NSC activity underlie this reduction. Particularly, increased NSC quiescence and consequently reduced NSC proliferation are considered to be major drivers of the low neurogenesis levels in the aged brain. Epigenetic regulators control the gene expression programs underlying NSC quiescence, proliferation and differentiation and are hence critical to the regulation of adult neurogenesis. Epigenetic alterations have also emerged as central hallmarks of aging, and recent studies suggest the deterioration of the NSC-specific epigenetic landscape as a driver of the age-dependent decline in adult neurogenesis. In this review, we summarize the recently accumulating evidence for a role of epigenetic dysregulation in NSC aging and propose perspectives for future research directions.
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650	_	7	\|a DNA methylation \|2 Other
650	_	7	\|a Lamin B1 \|2 Other
650	_	7	\|a aging \|2 Other
650	_	7	\|a chromatin \|2 Other
650	_	7	\|a epigenetic \|2 Other
650	_	7	\|a hippocampus \|2 Other
650	_	7	\|a histone \|2 Other
650	_	7	\|a neural stem cells \|2 Other
650	_	7	\|a neurogenesis \|2 Other
650	_	2	\|a Neurogenesis: physiology \|2 MeSH
650	_	2	\|a Cell Differentiation: genetics \|2 MeSH
650	_	2	\|a Neurons: metabolism \|2 MeSH
650	_	2	\|a Hippocampus: physiology \|2 MeSH
650	_	2	\|a Epigenesis, Genetic \|2 MeSH
700	1	_	\|a Toda, Tomohisa \|0 P:(DE-2719)2814117 \|b 1 \|e Last author \|u dzne
770	_	_	\|a Adult Neurogenesis in the Hippocampus
773	_	_	\|a 10.1002/hipo.23494 \|g p. hipo.23494 \|0 PERI:(DE-600)1498049-6 \|n 4 \|p 347-359 \|t Hippocampus \|v 33 \|y 2023 \|x 1050-9631
856	4	_	\|u https://pub.dzne.de/record/169366/files/DZNE-2023-00141.pdf \|y OpenAccess
856	4	_	\|u https://pub.dzne.de/record/169366/files/DZNE-2023-00141.pdf?subformat=pdfa \|x pdfa \|y OpenAccess
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910	1	_	\|a Deutsches Zentrum für Neurodegenerative Erkrankungen \|0 I:(DE-588)1065079516 \|k DZNE \|b 0 \|6 P:(DE-2719)2810548
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913	1	_	\|a DE-HGF \|b Gesundheit \|l Neurodegenerative Diseases \|1 G:(DE-HGF)POF4-350 \|0 G:(DE-HGF)POF4-352 \|3 G:(DE-HGF)POF4 \|2 G:(DE-HGF)POF4-300 \|4 G:(DE-HGF)POF \|v Disease Mechanisms \|x 0
914	1	_	\|y 2023
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Marc 21

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