| Literature DB >> 29673648 |
Quangdon Tran1, Jae-Hun Jung2, Jisoo Park1, Hyunji Lee1, Youngeun Hong1, Hyeonjeong Cho1, Minhee Kim1, Sungjin Park1, So-Hee Kwon3, Seon-Hwan Kim4, George Thomas5, Kwang Pyo Kim6, Myung-Haing Cho7, Jongsun Park8.
Abstract
Mitochondrial morphology, which is associated with changes in metabolism, cell cycle, cell development and cell death, is tightly regulated by the balance between fusion and fission. In this study, we found that S6 kinase 1 (S6K1) contributes to mitochondrial dynamics, homeostasis and function. Mouse embryo fibroblasts lacking S6K1 (S6K1-KO MEFs) exhibited more fragmented mitochondria and a higher level of Dynamin related protein 1 (Drp1) and active Drp1 (pS616) in both whole cell extracts and mitochondrial fraction. In addition, there was no evidence for autophagy and mitophagy induction in S6K1 depleted cells. Glycolysis and mitochondrial respiratory activity was higher in S6K1-KO MEFs, whereas OxPhos ATP production was not altered. However, inhibition of Drp1 by Mdivi1 (Drp1 inhibitor) resulted in higher OxPhos ATP production and lower mitochondrial membrane potential. Taken together the depletion of S6K1 increased Drp1-mediated fission, leading to the enhancement of glycolysis. The fission form of mitochondria resulted in lower yield for OxPhos ATP production as well as in higher mitochondrial membrane potential. Thus, these results have suggested a potential role of S6K1 in energy metabolism by modulating mitochondrial respiratory capacity and mitochondrial morphology.Entities:
Keywords: Drp1; Fission; Metabolic shift; Mitophagy; OxPhos; S6K1
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Year: 2018 PMID: 29673648 DOI: 10.1016/j.cellsig.2018.04.002
Source DB: PubMed Journal: Cell Signal ISSN: 0898-6568 Impact factor: 4.315