| Literature DB >> 27612012 |
Hyosun Tak1, Jung Woo Eun2, Jihye Kim3, So Jung Park4, Chongtae Kim1, Eunbyul Ji1, Heejin Lee1, Hoin Kang1, Dong-Hyung Cho4, Kyungbun Lee5, Wook Kim3, Suk Woo Nam2,6, Eun Kyung Lee1,6,7.
Abstract
Mitochondrial morphology is dynamically regulated by the formation of small fragmented units or interconnected mitochondrial networks, and this dynamic morphological change is a pivotal process in normal mitochondrial function. In the present study, we identified a novel regulator responsible for the regulation of mitochondrial dynamics. An assay using CHANG liver cells stably expressing mitochondrial-targeted yellow fluorescent protein (mtYFP) and a group of siRNAs revealed that T-cell intracellular antigen protein-1 (TIA-1) affects mitochondrial morphology by enhancing mitochondrial fission. The function of TIA-1 in mitochondrial dynamics was investigated through various biological approaches and expression analysis in human specimen. Downregulation of TIA-1-enhanced mitochondrial elongation, whereas ectopic expression of TIA-1 resulted in mitochondria fragmentation. In addition, TIA-1 increased mitochondrial activity, including the rate of ATP synthesis and oxygen consumption. Further, we identified mitochondrial fission factor (MFF) as a direct target of TIA-1, and showed that TIA-1 promotes mitochondrial fragmentation by enhancing MFF translation. TIA-1 null cells had a decreased level of MFF and less mitochondrial Drp1, a critical factor for mitochondrial fragmentation, thereby enhancing mitochondrial elongation. Taken together, our results indicate that TIA-1 is a novel factor that facilitates mitochondrial dynamics by enhancing MFF expression and contributes to mitochondrial dysfunction.Entities:
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Year: 2016 PMID: 27612012 PMCID: PMC5260506 DOI: 10.1038/cdd.2016.90
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 15.828