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MiR-31/SDHA Axis Regulates Reprogramming Efficiency through Mitochondrial Metabolism

Authors
Lee, Man RyulMantel, CharlieLee, Sang A.Moon, Sung-HwanBroxmeyer, Hal E.
Issue Date
12-Jul-2016
Publisher
Cell Press
Keywords
iPS; metabolism; reprogramming
Citation
Stem Cell Reports, v.7, no.1, pp 1 - 10
Pages
10
Journal Title
Stem Cell Reports
Volume
7
Number
1
Start Page
1
End Page
10
URI
https://scholarworks.bwise.kr/sch/handle/2021.sw.sch/8937
DOI
10.1016/j.stemcr.2016.05.012
ISSN
2213-6711
Abstract
Metabolism is remodeled when somatic cells are reprogrammed into induced pluripotent stem cells (iPSCs), but the majority of iPSCs are not fully reprogrammed. In a shift essential for reprogramming, iPSCs use less mitochondrial respiration but increased anaerobic glycolysis for bioenergetics. We found that microRNA 31 (miR-31) suppressed succinate dehydrogenase complex subunit A (SDHA) expression, vital for mitochondrial electron transport chain (ETC) complex II. MiR-31 overexpression in partially reprogrammed iPSCs lowered SDHA expression levels and oxygen consumption rates to that of fully reprogrammed iPSCs, but did not increase the proportion of fully reprogrammed TRA1-60(+) cells in colonies unless miR-31 was co-transduced with Yamanaka factors, which resulted in a 2.7-fold increase in full reprogramming. Thus switching from mitochondrial respiration to glycolytic metabolism through regulation of the miR-31/SDHA axis is critical for lowering the reprogramming threshold. This is supportive of multi-stage reprogramming whereby metabolic remodeling is fundamental.
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