Drosophila pink1 is required for mitochondrial function and interacts genetically with parkin

Clark, Ira E.; Dodson, Mark K.; Jiang, Chenfanfu; Cao, Joseph; Huh, Jun R.; Seol, Jae Hong; Yoo, Soon Ji; Hay, Bruce A.; Guo, Ming

doi:10.1038/nature04779

Cited by 1,600 publications

(1,597 citation statements)

References 28 publications

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“…Although nigral degeneration is absent in parkin-deficient mice, they exhibit decreased striatal mitochondrial respiratory capacity and decreased levels of proteins involved in protection from oxidative stress [12]. In Drosophila, deficiency in the mitochondrial kinase PINK1 resembles the pathology associated with mutant parkin, and notably, PINK1 defects can be rescued by wild-type parkin overexpression [62][63][64]. This implies that these proteins function in a common pathway to maintain mitochondrial integrity and function.…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial translocation of α-synuclein is promoted by intracellular acidification

Cole

DiEuliis

Leo

et al. 2008

Experimental Cell Research

180

164

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Mitochondrial dysfunction plays a central role in the selective vulnerability of dopaminergic neurons in Parkinson's disease (PD) and is influenced by both environmental and genetic factors. Expression of the PD protein α-synuclein or its familial mutants often sensitizes neurons to oxidative stress and to damage by mitochondrial toxins. This effect is thought to be indirect, since little evidence physically linking α-synuclein to mitochondria has been reported. Here, we show that the distribution of α-synuclein within neuronal and non-neuronal cells is dependent on intracellular pH. Cytosolic acidification induces translocation of α-synuclein from the cytosol onto the surface of mitochondria. Translocation occurs rapidly under artificially-induced low pH conditions and as a result of pH changes during oxidative or metabolic stress. Binding is likely facilitated by low pH-induced exposure of the mitochondria-specific lipid cardiolipin. These results imply a direct role for α-synuclein in mitochondrial physiology, especially under pathological conditions, and in principle, link α-synuclein to other PD genes in regulating mitochondrial homeostasis.

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Section: Discussionmentioning

confidence: 99%

Mitochondrial translocation of α-synuclein is promoted by intracellular acidification

Cole

DiEuliis

Leo

et al. 2008

Experimental Cell Research

180

164

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“…Cellular and mitochondrial ATP contents were measured in freshly prepared whole cell lysates and mitochondrial suspensions from left ventricles (LVs) according to manufacturer's instructions using the ATP Bioluminescence Assay Kit HS II (Roche) 26, 27. Freshly excised LVs were chopped and homogenized using a hand‐driven glass/Teflon potter Elvehjem homogenizer (Wheaton) in cell lysis reagent provided in the kit on ice.…”

Section: Methodsmentioning

confidence: 99%

Aberrant Mitochondrial Fission Is Maladaptive in Desmin Mutation–Induced Cardiac Proteotoxicity

Alam

Abdullah

Aishwarya

et al. 2018

JAHA

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BackgroundDesmin filament proteins interlink the contractile myofibrillar apparatus with mitochondria, nuclei and the sarcolemma. Mutations in the human desmin gene cause cardiac disease, remodeling, and heart failure but the pathophysiological mechanisms remain unknown.Methods and ResultsCardiomyocyte‐specific overexpression of mutated desmin (a 7 amino acid deletion R172‐E178, D7‐Des Tg) causes accumulations of electron‐dense aggregates and myofibrillar degeneration associated with cardiac dysfunction. Though extensive studies demonstrated that these altered ultrastructural changes cause impairment of cardiac contractility, the molecular mechanism of cardiomyocyte death remains elusive. In the present study, we report that the D7‐Des Tg mouse hearts undergo aberrant mitochondrial fission associated with increased expression of mitochondrial fission regulatory proteins. Mitochondria isolated from D7‐Des Tg hearts showed decreased mitochondrial respiration and increased apoptotic cell death. Overexpression of mutant desmin by adenoviral infection in cultured cardiomyocytes led to increased mitochondrial fission, inhibition of mitochondrial respiration, and activation of cellular toxicity. Inhibition of mitochondrial fission by mitochondrial division inhibitor mdivi‐1 significantly improved mitochondrial respiration and inhibited cellular toxicity associated with D7‐Des overexpression in cardiomyocytes.ConclusionsAberrant mitochondrial fission results in mitochondrial respiratory defects and apoptotic cell death in D7‐Des Tg hearts. Inhibition of aberrant mitochondrial fission using mitochondrial division inhibitor significantly preserved mitochondrial function and decreased apoptotic cell death. Taken together, our study shows that maladaptive aberrant mitochondrial fission causes desminopathy‐associated cellular dysfunction.

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“…This difference may be due to the presence of CG12362, a recent duplicate of ariadne-1 (Marín and Ferrús 2002). On the other hand, parkin mutants are viable, although show some phenotype changes, caused by a general mitochondrial dysfunction (Greene et al 2003;Pesah et al 2004;Clark et al 2006;Park et al 2006;Yang et al 2006). For the other genes, there are no loss-offunction mutants described.…”

Section: Long-term Conservation Of Particular Rbr Genes and Functionamentioning

confidence: 99%

RBR Ubiquitin Ligases: Diversification and Streamlining in Animal Lineages

Marı́n

2009

J Mol Evol

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The patterns of emergence and disappearance in animal species of genes encoding RBR ubiquitin ligases are described. RBR genes can be classified into subfamilies (Parkin, Ariadne, Dorfin, ARA54, etc.) according to sequence and structural data. Here, I show that most animal-specific RBR subfamilies emerged early in animal evolution, and that ancient animals, before the cnidarian/ bilaterian split, had a set of RBR genes, which was as complex as the one currently found in mammals. However, some lineages (nematodes, dipteran insects) have recently suffered multiple losses, leading to a highly simplified set of RBR genes. Genes of a particular RBR subfamily, characterized by containing a helicase domain and so far found only in plants, are present also in some animal species. The meaning of these patterns of diversification and streamlining are discussed at the light of functional data. Extreme evolutionary conservation may be related to gene products having housekeeping functions.

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Drosophila pink1 is required for mitochondrial function and interacts genetically with parkin

Cited by 1,600 publications

References 28 publications

Mitochondrial translocation of α-synuclein is promoted by intracellular acidification

Mitochondrial translocation of α-synuclein is promoted by intracellular acidification

Aberrant Mitochondrial Fission Is Maladaptive in Desmin Mutation–Induced Cardiac Proteotoxicity

RBR Ubiquitin Ligases: Diversification and Streamlining in Animal Lineages

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