Defective mitochondrial fusion, altered respiratory function, and distorted cristae structure in skin fibroblasts with heterozygous OPA1 mutations
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- 作者:Virginie Agier ; Patricia Oliviero ; Jeanne Lain¨¦ ; Caroline L'Hermitte-Stead ; Samantha Girard ; S ; rine Fillaut ; Claude Jardel ; Fr¨¦d¨¦ric Bouillaud ; Anne Laure Bulteau ; Anne Lomb¨¨s
- 关键词:ADOA ; autosomal dominant optic atrophy ; AR ; aspect ratio ; cccp ; carbonyl cyanide m-chlorophenyl hydrazone ; ¦¤¦× ; mitochondrial inner membrane potential ; mtDNA ; mitochondrial DNA ; OXPHOS ; oxidative phosphorylation ; SOD1 ; Cu ; Zn-superoxide dismutase ; SOD2 ; M
- 刊名:Biochimica et Biophysica Acta (BBA)/Molecular Basis of Disease
- 出版年:2012
- 出版时间:October, 2012
- 年:2012
- 卷:1822
- 期:10
- 页码:1570-1580
- 全文大小:1997 K
文摘
Deleterious consequences of heterozygous OPA1 mutations responsible for autosomal dominant optic atrophy remain a matter of debate. Primary skin fibroblasts derived from patients have shown diverse mitochondrial alterations that were however difficult to resolve in a unifying scheme. To address the potential use of these cells as disease model, we undertook parallel and quantitative analyses of the diverse reported alterations in four fibroblast lines harboring different OPA1 mutations, nonsense or missense, in the guanosine triphosphatase or the C-terminal coiled-coil domains. We tackled several factors potentially underlying discordant reports and showed that fibroblasts with heterozygous OPA1 mutations present with several mitochondrial alterations. These included defective mitochondrial fusion during pharmacological challenge with the protonophore carbonyl cyanide m©\chlorophenyl hydrazone, significant mitochondrial elongation with decreased OPA1 and DRP1 proteins, and abnormal mitochondrial fragmentation during glycolysis shortage or exogenous oxidative stress. Respiratory complex IV activity and subunits steady-state were decreased without alteration of the mitochondrial deoxyribonucleic acid size, amount or transcription. Physical link between OPA1 protein and oxidative phosphorylation was shown by reciprocal immunoprecipitation. Altered cristae structure coexisted with normal response to pro-apoptotic stimuli and expression of Bax or Bcl2 proteins. Skin fibroblasts with heterozygous OPA1 mutations thus share significant mitochondrial remodeling, and may therefore be useful for analyzing disease pathophysiology. Identifying whether the observed alterations are also present in ganglion retinal cells, and which of them underlies their degeneration process remains however an essential goal for therapeutic strategy.