OPA1‐dependent cristae modulation is essential for cellular adaptation to metabolic demand

Patten, David A.; Wong, Jacob; Khacho, Mireille; Soubannier, Vincent; Mailloux, Ryan J.; Pilon-Larose, Karine; MacLaurin, Jason G.; Park, David; McBride, Heidi M.; Trinkle-Mulcahy, Laura; Harper, Mary‐Ellen; Germain, Marc; Slack, Ruth S.

doi:10.15252/embj.201488349

Cited by 335 publications

(361 citation statements)

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“…These results indicate that StarD7 is important for mitochondrial ATP generation and cell growth. These phenotypes of StarD7-KO cells were similar to the cells having optic atrophy 1 (Opa1) deficiency, which is an important protein for the maintenance of cristae architecture (13).…”

Section: Stard7 Maintains Mitochondrial Phosphatidylcholine Compositionmentioning

confidence: 62%

“…Analysis of Opa1 Oligomerization-Opa1 oligomerization was analyzed as described before (13). Briefly, after washing with PBS, cells were treated with 1 mM bismaleimidohexane (Thermo Fisher Scientific), a cell-permeable cross-linker, for 20 min at 37°C.…”

Section: Methodsmentioning

confidence: 99%

“…The inner membrane dynamin-like GTPase Opa1 mediates inner membrane mitochondrial fusion and morphology (13,15,16). Inner membrane proteases such as Oma1 cleave long membrane-bound Opa1 forms (Opa1-L) into short soluble forms (Opa1-S).…”

Section: Journal Of Biological Chemistry 24883mentioning

confidence: 99%

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StarD7 Protein Deficiency Adversely Affects the Phosphatidylcholine Composition, Respiratory Activity, and Cristae Structure of Mitochondria

Horibata

Ando

Zhang

et al. 2016

Journal of Biological Chemistry

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Edited by Dennis VoelkerPhosphatidylcholine (PC) is a major phospholipid of mitochondria, comprising 40 -50% of both the outer and the inner membranes. However, PC must be imported from its production organelles because mitochondria lack the enzymes essential for PC biosynthesis. In a previous study, we found that StarD7 mediates the intracellular transfer of PC to mitochondria. Therefore, in this study, we analyzed the contribution of StarD7 to the maintenance of mitochondrial phospholipid content and function using siRNA-mediated knockdown and knock-out (KO) of the StarD7 gene in HEPA-1 cells. Real time analysis of respiratory activity demonstrated that the oxygen consumption rate and activity of mitochondrial complexes were impaired in StarD7-KD cells. To confirm these results, we established StarD7-KO HEPA-1 cells by double nicking using CRISPR/Cas9n. As expected, StarD7-KD and -KO cells showed a significant reduction in mitochondrial PC content. The ATP level and growth rate of KO cells were notably lower compared with wild-type cells when cultured in glucose-free galactosecontaining medium to force cells to rely on mitochondrial ATP production. In KO cells, the level of the MTCO1 protein, a primary subunit of complex IV, was reduced without a concomitant decrease in its mRNA, but the level was restored when StarD7-I was overexpressed. StarD7-KO cells showed impaired formation of the mitochondrial supercomplexes and exhibited a disorganized cristae structure, with no changes in optic atrophy 1 protein. These findings indicate that StarD7 plays important roles in maintaining the proper composition of mitochondrial phospholipids as well as mitochondrial function and morphogenesis.

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Section: Stard7 Maintains Mitochondrial Phosphatidylcholine Compositionmentioning

confidence: 62%

Section: Methodsmentioning

confidence: 99%

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StarD7 Protein Deficiency Adversely Affects the Phosphatidylcholine Composition, Respiratory Activity, and Cristae Structure of Mitochondria

Horibata

Ando

Zhang

et al. 2016

Journal of Biological Chemistry

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“…1G, Hoechst), and AKO animals had normal numbers of neurons in layer V (28). Similar SOD1-negative vacuoles were observed in MEFs lacking the mitochondrial inner membrane GTPase OPA1, 4 a protein required for mitochondrial fusion, and to maintain cristae structure (31,37,38). Together, these results indicate that inhibition of mitochondrial function causes the occurrence of large intracytoplasmic vacuoles.…”

Section: Mitochondrial Dysfunction Causes the Appearance Of Largementioning

confidence: 72%

Loss of Mitochondrial Function Impairs Lysosomes

Demers-Lamarche

Guillebaud

Tlili

et al. 2016

Journal of Biological Chemistry

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198

193

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Alterations in mitochondrial function, as observed in neurodegenerative diseases, lead to disrupted energy metabolism and production of damaging reactive oxygen species. Here, we demonstrate that mitochondrial dysfunction also disrupts the structure and function of lysosomes, the main degradation and recycling organelle. Specifically, inhibition of mitochondrial function, following deletion of the mitochondrial protein AIF, OPA1, or PINK1, as well as chemical inhibition of the electron transport chain, impaired lysosomal activity and caused the appearance of large lysosomal vacuoles. Importantly, our results show that lysosomal impairment is dependent on reactive oxygen species. Given that alterations in both mitochondrial function and lysosomal activity are key features of neurodegenerative diseases, this work provides important insights into the etiology of neurodegenerative diseases.A prominent feature of neurodegenerative diseases, including Parkinson disease (PD) 3 and Alzheimer disease, is the accumulation of undigested protein aggregates (1, 2). Although the underlying mechanisms are complex, several cellular alterations can cause aggregate accumulation, including impaired quality control pathways and the generation of reactive oxygen species (ROS) as a consequence of mitochondrial damage (1, 3).In healthy cells, protein aggregates and damaged cellular components are delivered to lysosomes to be degraded through a process termed autophagy (1, 2, 4, 5). As such, autophagy plays an important neuroprotective role. Nevertheless, the defects in degradation pathways observed in neurodegenerative diseases extend well beyond alterations in autophagy. Specifically, disruption of lysosomal function has been linked to neuronal loss in several neurodegenerative diseases. For example, mutations in the lysosomal ATPase ATP13A2 cause PD, whereas lysosomal dysfunction in Gaucher disease leads to Parkinsonism and the appearance of Lewy bodies (6, 7). In addition, the ␣-synuclein-containing Lewy bodies found in PD are positive for lysosomal markers, suggesting that they represent lysosomes that failed to degrade their content (8). In fact, lysosomal alterations are a common feature of PD (8 -11). Nevertheless, the pathological consequences of a loss of lysosomal function extend well beyond PD, because a wide variety of mutations that impair lysosomes and cause the accumulation of intracellular material (lysosomal storage diseases) show features of neurodegeneration (12).A second key metabolic pathway required for neuronal survival is mitochondrial activity. In fact, mitochondrial dysfunction is a common feature of neurodegenerative diseases. For example, decreased activity of complex I of the electron transport chain (ETC) is present in a number of PD cases (13, 14), whereas amyloid ␤, Tau tangles, and Htt aggregates all cause mitochondrial dysfunction (15-17). In addition, several genes mutated in PD (including PINK1, Parkin, and DJ-1) affect mitochondrial function and turnover (18 -21), whereas deregulation of mitochon...

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“…Downregulation of Mfns or Opa-1 levels reduces OXPHOS and ATP production in several cell models [81][82][83]. In line with this, Opa-1-driven cristae remodelling is strictly required for regulating ATP production upon different cell needs [84], while Mfn-2 overexpression in myotubes can upregulate the transcription of OXPHOS genes [85]. However, in HeLa cells, prolonged Drp1 downregulation can reduce respiration levels [86], this suggesting that optimal OXPHOS activity requires a balanced equilibrium in mitochondrial morphology.…”

Section: Mitochondrial Dynamics and Cell Metabolismmentioning

confidence: 78%

The mitochondrial dynamics in cancer and immune-surveillance

Simula

Nazio

Campello

2017

Seminars in Cancer Biology

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A B S T R A C TMitochondria-shaping proteins control the dynamic equilibrium between fusion and fission of the mitochondrial network. Their balance is strictly required to regulate various processes, including the quality of mitochondria, cell metabolism, cell death, proliferation and cell migration. Alterations in these processes are frequently encountered in cancer, during both its onset and later progression, as evidence emerge connecting alterations in mitochondrial dynamics with cancer development. In recent years, novel therapeutic approaches to fight against different human tumors aim at exploiting the immune system's ability to specifically recognize tumor antigens, thus killing malignant cells in a process named immune-surveillance. Interestingly, data are accumulating on the role that mitochondrial dynamics play also for the correct function of both the innate and the adaptive immune system. By this review, we overview how mitochondrial dynamics can affect various processes during cancer development, acting directly on tumor cells or indirectly on cells responsible for tumor aggression and defence.

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OPA1‐dependent cristae modulation is essential for cellular adaptation to metabolic demand

Cited by 335 publications

References 50 publications

StarD7 Protein Deficiency Adversely Affects the Phosphatidylcholine Composition, Respiratory Activity, and Cristae Structure of Mitochondria

StarD7 Protein Deficiency Adversely Affects the Phosphatidylcholine Composition, Respiratory Activity, and Cristae Structure of Mitochondria

Loss of Mitochondrial Function Impairs Lysosomes

The mitochondrial dynamics in cancer and immune-surveillance

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