Loss of the Parkinson's disease-linked gene DJ-1 perturbs mitochondrial dynamics

Irrcher, Isabella; Aleyasin, Hossein; Seifert, Erin L.; Hewitt, Sarah J.; Chhabra, Shivani; Phillips, Maryam; Lutz, A. Kathrin; Rousseaux, Maxime W.C.; Bevilacqua, Lisa; Jahani‐Asl, Arezu; Callaghan, Steve; MacLaurin, Jason G.; Winklhofer, Konstanze F.; Rizzu, Patrizia; Rippstein, Peter; Kim, Raymond H.; Chen, C.X.; Fon, Edward A.; Slack, Ruth S.; Harper, Mary‐Ellen; McBride, Heidi M.; Mak, Tak W.; Park, David

doi:10.1093/hmg/ddq288

Cited by 344 publications

(287 citation statements)

References 65 publications

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“…However, PINK1 or Parkin overexpression rescues the aberrant mitochondrial phenotype in DJ-1-deficient cells, but DJ-1 does not reduce the mitochondrial fragmentation induced by PINK1 deficiency. These findings suggest that DJ-1 acts independent of PINK1 and Parkin (Exner et al, 2007;Irrcher et al, 2010;Thomas et al, 2011).…”

Section: Other Mitochondrial Partners Of Pink1 In Mitochondrial Protementioning

confidence: 78%

PINK1 as a Molecular Checkpoint in the Maintenance of Mitochondrial Function and Integrity

Koh

Chung

2012

Molecules and Cells

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Parkinson's disease (PD), the most prevalent neurodegenerative movement disorder, is characterized by an agedependent selective loss of dopaminergic (DA) neurons. Although most PD cases are sporadic, more than 20 responsible genes in familial cases were identified recently. Genetic studies using Drosophila models demonstrate that PINK1, a mitochondrial kinase encoded by a PD-linked gene PINK1, is critical for maintaining mitochondrial function and integrity. This suggests that mitochondrial dysfunction is the main cause of PD pathogenesis. Further genetic and cell biological studies revealed that PINK1 recruits Parkin, an E3 ubiquitin ligase encoded by another PD-linked gene parkin, to mitochondria and regulates the mitochondrial remodeling process via the Parkin-mediated ubiquitination of various mitochondrial proteins. PINK1 also directly phosphorylates the mitochondrial proteins Miro and TRAP1, subsequently inhibiting mitochondrial transport and mitochondrial oxidative damage, respectively. Moreover, recent Drosophila genetic analyses demonstrate that the neuroprotective molecules Sir2 and FOXO specifically complement mitochondrial dysfunction and DA neuron loss in PINK1 null mutants, suggesting that Sir2 and FOXO protect mitochondria and DA neurons downstream of PINK1. Collectively, these recent results suggest that PINK1 plays multiple roles in mitochondrial quality control by regulating its mitochondrial, cytosolic, and nuclear targets.

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Section: Other Mitochondrial Partners Of Pink1 In Mitochondrial Protementioning

confidence: 78%

PINK1 as a Molecular Checkpoint in the Maintenance of Mitochondrial Function and Integrity

Koh

Chung

2012

Molecules and Cells

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“…S5). Human DJ-1 has been previously associated with autophagy, but its precise role is controversial (35)(36)(37). Although no association between members of the Hsp31 minifamily and RNA metabolism has been described, human DJ-1 is an RNA binding protein (38), suggesting this cellular function may be conserved.…”

Section: Discussionmentioning

confidence: 99%

Yeast DJ-1 superfamily members are required for diauxic-shift reprogramming and cell survival in stationary phase

Miller-Fleming

Antas

Pais

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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The yeast Hsp31 minifamily proteins (Hsp31, Hsp32, Hsp33, Hsp34) belong to the highly conserved DJ-1 superfamily. The human DJ-1 protein is associated with cancer and neurodegenerative disorders, such as Parkinson disease. However, the precise function of human and yeast DJ-1 proteins is unclear. Here we show that the yeast DJ-1 homologs have a role in diauxic-shift (DS), characterized by metabolic reprogramming because of glucose limitation. We find that the Hsp31 genes are strongly induced in DS and in stationary phase (SP), and that deletion of these genes reduces chronological lifespan, impairs transcriptional reprogramming at DS, and impairs the acquisition of several typical characteristics of SP, including autophagy induction. In addition, under carbon starvation, the HSP31 family gene-deletion strains display impaired autophagy, disrupted target of rapamycin complex 1 (TORC1) localization to P-bodies, and caused abnormal TORC1-mediated Atg13 phosphorylation. Repression of TORC1 by rapamycin in the gene-deletion strains completely reversed their sensitivity to heat shock. Taken together, our data indicate that Hsp31 minifamily is required for DS reprogramming and cell survival in SP, and plays a role upstream of TORC1. The enhanced understanding of the cellular function of these genes sheds light into the biological role of other members of the superfamily, including DJ-1, which is an attractive target for therapeutic intervention in cancer and in Parkinson disease.

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“…Consequently, the irreversible binding of mutant a-synuclein to the lysosome blocks the binding of other substrates, resulting in a general impairment of the CMA pathway and further a-synuclein accumulation 110 . Proteins related to familiar PD, such as DJ-1 or LRRK2, significantly alter autophagy 111,112 .…”

Section: Loss Of Clearance Mechanisms As a Determinant Of Ageingmentioning

confidence: 99%

The role of protein clearance mechanisms in organismal ageing and age-related diseases

2014

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Loss of the Parkinson's disease-linked gene DJ-1 perturbs mitochondrial dynamics

Cited by 344 publications

References 65 publications

PINK1 as a Molecular Checkpoint in the Maintenance of Mitochondrial Function and Integrity

PINK1 as a Molecular Checkpoint in the Maintenance of Mitochondrial Function and Integrity

Yeast DJ-1 superfamily members are required for diauxic-shift reprogramming and cell survival in stationary phase

The role of protein clearance mechanisms in organismal ageing and age-related diseases

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