The C. elegans Opa1 Homologue EAT-3 Is Essential for Resistance to Free Radicals

Mitochondria are key regulators of cell viability and provide essential functions that protect against neurodegenerative disease. To develop a model for mitochondrial-dependent neurodegeneration in Caenorhabditis elegans, we used RNA interference (RNAi) and genetic ablation to knock down expression of enzymes in the Coenzyme Q (CoQ) biosynthetic pathway. CoQ is a required component of the ATP-producing electron transport chain in mitochondria. We found that reduced levels of CoQ result in a progressive uncoordinated (Unc) phenotype that is correlated with the appearance of degenerating GABA neurons. Both the Unc and degenerative phenotypes emerge during late larval development and progress in adults. Neuron classes in motor and sensory circuits that use other neurotransmitters (dopamine, acetylcholine, glutamate, serotonin) and body muscle cells were less sensitive to CoQ depletion. Our results indicate that the mechanism of GABA neuron degeneration is calcium-dependent and requires activation of the apoptotic gene, ced-4 (Apaf-1). A molecular cascade involving mitochondrial-initiated cell death is also consistent with our finding that GABA neuron degeneration requires the mitochondrial fission gene, drp-1. We conclude that the cell selectivity and developmental progression of CoQ deficiency in C. elegans indicate that this model may be useful for delineating the role of mitochondrial dysfunction in neurodegenerative disease.cell death | disease | mitochondria | neurodegeneration | necrosis

Section: Coq-1 Knockdown-induced Cell Death Depends On the Mitochondrialmentioning

confidence: 89%

Coenzyme Q protects Caenorhabditis elegans GABA neurons from calcium-dependent degeneration

Earls

Hacker²,

Watson³

et al. 2010

“…Their C. elegans homologs are drp-1, fzo-1, and eat-3, respectively (28)(29)(30). We examined mitochondrial morphology in the drp-1 null mutant, and found that age-dependent mitochondrial fragmentation in the drp-1 mutant was similar to that of the wild type ( Fig.…”

Section: Drp-1-mediated Mitochondrial Defects In Activity-deficient Nmentioning

confidence: 95%

Neural activity and CaMKII protect mitochondria from fragmentation in aging Caenorhabditis elegans neurons

Jiang

Hsu

Yen

et al. 2015

Decline in mitochondrial morphology and function is a hallmark of neuronal aging. Here we report that progressive mitochondrial fragmentation is a common manifestation of aging Caenorhabditis elegans neurons and body wall muscles. We show that sensoryevoked activity was essential for maintaining neuronal mitochondrial morphology, and this activity-dependent mechanism required the Degenerin/ENaC sodium channel MEC-4, the L-type voltagegated calcium channel EGL-19, and the Ca/calmodulin-dependent kinase II (CaMKII) UNC-43. Importantly, UNC-43 phosphorylated and inhibited the dynamin-related protein (DRP)-1, which was responsible for excessive mitochondrial fragmentation in neurons that lacked sensory-evoked activity. Moreover, enhanced activity in the aged neurons ameliorated mitochondrial fragmentation. These findings provide a detailed description of mitochondrial behavior in aging neurons and identify activity-dependent DRP-1 phosphorylation by CaMKII as a key mechanism in neuronal mitochondrial maintenance. mitochondria | neuronal aging | neural activity | C. elegans | CaMKII

“…In C. elegans, FZO-1 and EAT-3 are required for the fusion of the outer mitochondrial membrane and the inner mitochondrial membrane, respectively (7,(10)(11)(12)(13). To determine whether mitochondrial hyperfusion induced by mma-1(RNAi) is dependent on these GTPases, we performed RNAi experiments in animals carrying a null-mutation in the fzo-1 gene [fzo-1(tm1133)] or the eat-3 gene [eat-3(tm1107)].…”

Section: Reducing Complex IV But Not Complex I Assembly Induces Mitocmentioning

confidence: 99%

“…For example, mammalian Drp1 or Caenorhabditis elegans DRP-1 are required for mitochondrial fission (6,7). Conversely, mammalian Mfn1/2 and Opa1 or C. elegans FZO-1 and EAT-3 are required for the fusion of the outer and inner mitochondrial membrane, respectively (8)(9)(10)(11)(12)(13).…”

mentioning

confidence: 99%

Impaired complex IV activity in response to loss of LRPPRC function can be compensated by mitochondrial hyperfusion

Rolland

Motori

Memar

et al. 2013

Mitochondrial morphology changes in response to various stimuli but the significance of this is unclear. In a screen for mutants with abnormal mitochondrial morphology, we identified MMA-1, the Caenorhabditis elegans homolog of the French Canadian Leigh Syndrome protein LRPPRC (leucine-rich pentatricopeptide repeat containing). We demonstrate that reducing mma-1 or LRPPRC function causes mitochondrial hyperfusion. Reducing mma-1/ LRPPRC function also decreases the activity of complex IV of the electron transport chain, however without affecting cellular ATP levels. Preventing mitochondrial hyperfusion in mma-1 animals causes larval arrest and embryonic lethality. Furthermore, prolonged LRPPRC knock-down in mammalian cells leads to mitochondrial fragmentation and decreased levels of ATP. These findings indicate that in a mma-1/LRPPRC-deficient background, hyperfusion allows mitochondria to maintain their functions despite a reduction in complex IV activity. Our data reveal an evolutionary conserved mechanism that is triggered by reduced complex IV function and that induces mitochondrial hyperfusion to transiently compensate for a drop in the activity of the electron transport chain.mitochondrial dynamics | cytochrome c oxidase deficiency neurodegeneration