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Mitochondrial fission and fusion mediators, hFis1 and OPA1, modulate cellular senescence.

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dc.contributor.authorLee, S-
dc.contributor.authorJeong, SY-
dc.contributor.authorLim, WC-
dc.contributor.authorKim, S-
dc.contributor.authorPark, YY-
dc.contributor.authorSun, X-
dc.contributor.authorYoule, RJ-
dc.contributor.authorCho, H-
dc.date.accessioned2011-01-19T01:49:57Z-
dc.date.available2011-01-19T01:49:57Z-
dc.date.issued2007-
dc.identifier.issn0021-9258-
dc.identifier.urihttp://repository.ajou.ac.kr/handle/201003/1209-
dc.description.abstractThe number and morphology of mitochondria within a cell are precisely regulated by the mitochondrial fission and fusion machinery. The human protein, hFis1, participates in mitochondrial fission by recruiting the Drp1 into the mitochondria. Using short hairpin RNA, we reduced the expression levels of hFis1 in mammalian cells. Cells lacking hFis1 showed sustained elongation of mitochondria and underwent significant cellular morphological changes, including enlargement, flattening, and increased cellular granularity. In these cells, staining for acidic senescence-associated beta-galactosidase activity was elevated, and the rate of cell proliferation was greatly reduced, indicating that cells lacking hFis1 undergo senescence-associated phenotypic changes. Reintroduction of the hFis1 gene into hFis1-depleted cells restored mitochondrial fragmentation and suppressed senescence-associated beta-galactosidase activity. Moreover, depletion of both hFis1 and OPA1, a critical component of mitochondrial fusion, resulted in extensive mitochondrial fragmentation and markedly rescued cells from senescence-associated phenotypic changes. Intriguingly, sustained elongation of mitochondria was associated with decreased mitochondrial membrane potential, increased reactive oxygen species production, and DNA damage. The data indicate that sustained mitochondrial elongation induces senescence-associated phenotypic changes that can be neutralized by mitochondrial fragmentation. Thus, one of the key functions of mitochondrial fission might be prevention of the sustained extensive mitochondrial elongation that triggers cellular senescence.-
dc.language.isoen-
dc.subject.MESHCell Aging-
dc.subject.MESHCell Proliferation-
dc.subject.MESHDNA Damage-
dc.subject.MESHDNA Fragmentation-
dc.subject.MESHGTP Phosphohydrolases-
dc.subject.MESHGene Silencing-
dc.subject.MESHHela Cells-
dc.subject.MESHHumans-
dc.subject.MESHMembrane Proteins-
dc.subject.MESHMitochondria-
dc.subject.MESHMitochondrial Proteins-
dc.subject.MESHModels, Biological-
dc.subject.MESHPhenotype-
dc.subject.MESHRNA Interference-
dc.subject.MESHReactive Oxygen Species-
dc.subject.MESHTime Factors-
dc.titleMitochondrial fission and fusion mediators, hFis1 and OPA1, modulate cellular senescence.-
dc.typeArticle-
dc.identifier.pmid17545159-
dc.identifier.urlhttp://www.jbc.org/cgi/pmidlookup?view=long&pmid=17545159-
dc.contributor.affiliatedAuthor정, 선용-
dc.contributor.affiliatedAuthor김, 수정-
dc.contributor.affiliatedAuthor조, 혜성-
dc.type.localJournal Papers-
dc.identifier.doi10.1074/jbc.M700679200-
dc.citation.titleThe Journal of biological chemistry-
dc.citation.volume282-
dc.citation.number31-
dc.citation.date2007-
dc.citation.startPage22977-
dc.citation.endPage22983-
dc.identifier.bibliographicCitationThe Journal of biological chemistry, 282(31). : 22977-22983, 2007-
dc.identifier.eissn1083-351X-
dc.relation.journalidJ000219258-
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Medical Genetics
Journal Papers > School of Medicine / Graduate School of Medicine > Biochemistry & Molecular Biology
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