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Mitochondrial quality control: Cell-type-dependent responses to pathological mutant mitochondrial DNA
Authors:Adriana Malena  Boris Pantic  Doriana Borgia  Gianluca Sgarbi  Giancarlo Solaini  Ian J Holt
Institution:1. Department of Neurosciences, University of Padova, Italy;2. Department of Biomedical and Neuromotor Sciences, University of Bologna, Italy;3. Medical Research Council, Mill Hill Laboratory, London, United Kingdom
Abstract:Pathological mutations in the mitochondrial DNA (mtDNA) produce a diverse range of tissue-specific diseases and the proportion of mutant mitochondrial DNA can increase or decrease with time via segregation, dependent on the cell or tissue type. Previously we found that adenocarcinoma (A549.B2) cells favored wild-type (WT) mtDNA, whereas rhabdomyosarcoma (RD.Myo) cells favored mutant (m3243G) mtDNA. Mitochondrial quality control (mtQC) can purge the cells of dysfunctional mitochondria via mitochondrial dynamics and mitophagy and appears to offer the perfect solution to the human diseases caused by mutant mtDNA. In A549.B2 and RD.Myo cybrids, with various mutant mtDNA levels, mtQC was explored together with macroautophagy/autophagy and bioenergetic profile. The 2 types of tumor-derived cell lines differed in bioenergetic profile and mitophagy, but not in autophagy. A549.B2 cybrids displayed upregulation of mitophagy, increased mtDNA removal, mitochondrial fragmentation and mitochondrial depolarization on incubation with oligomycin, parameters that correlated with mutant load. Conversely, heteroplasmic RD.Myo lines had lower mitophagic markers that negatively correlated with mutant load, combined with a fully polarized and highly fused mitochondrial network. These findings indicate that pathological mutant mitochondrial DNA can modulate mitochondrial dynamics and mitophagy in a cell-type dependent manner and thereby offer an explanation for the persistence and accumulation of deleterious variants.
Keywords:A549  B2 adenocarcinoma cells  autophagy  mitochondria  mitochondrial dynamics  mitochondrial quality control  mitophagy  mutation-m3243G  pathological mtDNA  RD  Myo rhabdomyosarcoma cells
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