Association of PINK1 and DJ-1 confers digenic inheritance of early-onset Parkinson's disease

Tang, Beisha; Xiong, Hui; Sun, Peng; Zhang, Yuhu; Wang, Danling; Hu, Zhengmao; Zhu, Zanhua; Ma, Hong; Pan, Qian; Xia, Jiahui; Xia, Kun; Zhang, Zhuohua

doi:10.1093/hmg/ddl104

Cited by 205 publications

(152 citation statements)

References 50 publications

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“…Functional studies suggest that wildtype PINK1 may have a neuroprotective role (4) that is abrogated by pathogenic mutations in the PINK1 gene. Consistent with the notion, we have recently shown that PINK1 and DJ-1 physically associate and collaborate to protect cells against oxidative stress (15). These results suggest a potential role of PINK1 in maintaining mitochondrial homeostasis and in defending against oxidative stress.…”

supporting

confidence: 80%

“…In vitro, parkin and DJ-1 have been shown to protect cells from oxidative stress (26)(27)(28)(29)(30)(31). Moreover, PINK1 interacts with DJ-1 and digenic mutations of PINK1 and DJ-1 are associated in early onset familial form of PD (15). Consistent with our findings that antioxidants can ameliorate the dPINK1-dependent PD pathology in Drosophila are two recent reports that show that deletion mutants of dPINK1 result in abnormally functioning mitochondria, sensitization to oxidative stress, and mild degeneration of DA neurons (32,33).…”

Section: Aј-dј and E)mentioning

confidence: 99%

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Antioxidants protect PINK1 -dependent dopaminergic neurons in Drosophila

Wang

Xiong

et al. 2006

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

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Parkinson's disease (PD) is the most frequent neurodegenerative movement disorder. Mutations in the PINK1 gene are linked to the autosomal recessive early onset familial form of PD. The physiological function of PINK1 and pathological abnormality of PDassociated PINK1 mutants are largely unknown. We here show that inactivation of Drosophila PINK1 (dPINK1) using RNAi results in progressive loss of dopaminergic neurons and in ommatidial degeneration of the compound eye, which is rescued by expression of human PINK1 (hPINK1). Expression of human SOD1 suppresses neurodegeneration induced by dPINK1 inactivation. Moreover, treatment of dPINK1 RNAi flies with the antioxidants SOD and vitamin E significantly inhibits ommatidial degeneration. Thus, dPINK1 plays an essential role in maintaining neuronal survival by preventing neurons from undergoing oxidative stress, thereby suggesting a potential mechanism by which a reduction in PINK1 function leads to PD-associated neurodegeneration.neurodegeneration ͉ oxidative stress ͉ Parkinson's disease ͉ SOD1

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supporting

confidence: 80%

Section: Aј-dј and E)mentioning

confidence: 99%

Antioxidants protect PINK1 -dependent dopaminergic neurons in Drosophila

Wang

Xiong

et al. 2006

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

Self Cite

185

140

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“…14-3-3E is a member of the 14-3-3 family of phosphoserine-binding adapter molecules that mediate a general survival-promoting function through interaction with target proteins, by enhancing pro-survival signalling while suppressing activity of proapoptotic proteins (Porter et al, 2006). PINK1 encodes a Ser/ Thr kinase with a mitochondrial-targeting signal, and acts with DJ-1 to protect cells against oxidative stress-induced cell death (Tang et al, 2006).…”

Section: Discussionmentioning

confidence: 99%

Myostatin inactivation induces a similar muscle molecular signature in double-muscled cattle as in mice

Chelh

Picard

Hocquette

et al. 2011

Animal

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Myostatin (MSTN), a member of the TGF-b superfamily, is a negative regulator of skeletal muscle mass. We have previously shown that the cell survival/apoptosis pathway is a downstream target of MSTN loss-of-function in mice through the regulation of the expression or abundance of many survival and apoptotic factors. In this study, we used western-blot and quantitative PCR (qPCR) analyses to validate these novel downstream targets of MSTN in double-muscled (DM) cattle v. their controls including 260-day-old foetuses and adult cows from the INRA95 strain. MSTN loss-of-function in DM foetuses and DM cows resulted in a glycolytic shift of the muscles (e.g. upregulation of H-MyBP, PGM1 and SNTA1 and downregulation of H-FABP), activation of cell survival pathway through regulation of some components of the PI3K/Akt pathway (e.g. upregulation of DJ-1 and Gsk-3bser9/ Gsk-3btotal ratio and downregulation of PTEN) and upregulation of cell survival factors translationally controlled tumour protein (14-3-3E, Pink1). We also found a lower abundance of pro-apoptotic transcripts and/or proteins (Caspase-3, caspase-8, caspase-9, BID, ID2 and Daxx) and a higher expression of anti-apoptotic transcripts (Traf2 and Bcl2l2) in DM muscles. All together, these results are in favour of activation of the cell survival pathway and loss of apoptosis pathway within the muscles of DM animals. Alteration of both pathways may increase myonuclear or satellite cell survival, which is crucial for protein synthesis. This could contribute to muscle hypertrophy in DM foetuses and DM cows.Keywords: myostatin, cattle, muscle hypertrophy, apoptosis, cell survival ImplicationsMuscle hypertrophy has been extensively studied in meatproducing animals. In double-muscled (DM) cattle, a loss-offunction mutation in the myostatin gene (MSTN ) is responsible for muscle hypertrophy. In order to get a thorough knowledge of the molecular mechanisms of MSTN action, we have examined the molecular phenotype of DM muscle based on our previous data in MSTN-null mice. The data bring new elements to the understanding of the DM muscle phenotype and of the regulation of muscle mass in farm animals.

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“…Consistent with this notion, a recent study reports that digenic mutations of PINK1 and DJ-1 are associated with early-onset familial PD cases (10). In addition, expression of these two pathogenic proteins potentiates susceptibility of SH-SY5Y cells to oxidative stress, and PINK1 and DJ-1 can form a complex when coexpressed in mammalian cells (10). PINK1 and DJ-1 appear to function in the same pathway as Parkin, which encodes an E3 ubiquitin ligase that is thought to function primarily in the cytoplasm, presumably to target specific protein targets for degradation or modified function͞local-ization (11).…”

Section: The Parkinson Pathwaymentioning

confidence: 59%

“…PINK1 is likely to function in conjunction with another mitochondrial protein known as DJ-1 because mutations in this gene also cause autosomal recessive forms of PD. Consistent with this notion, a recent study reports that digenic mutations of PINK1 and DJ-1 are associated with early-onset familial PD cases (10). In addition, expression of these two pathogenic proteins potentiates susceptibility of SH-SY5Y cells to oxidative stress, and PINK1 and DJ-1 can form a complex when coexpressed in mammalian cells (10).…”

Section: The Parkinson Pathwaymentioning

confidence: 80%

Antioxidants put Parkinson flies back in the PINK

Bier

2006

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

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Association of PINK1 and DJ-1 confers digenic inheritance of early-onset Parkinson's disease

Cited by 205 publications

References 50 publications

Antioxidants protect PINK1 -dependent dopaminergic neurons in Drosophila

Antioxidants protect PINK1 -dependent dopaminergic neurons in Drosophila

Myostatin inactivation induces a similar muscle molecular signature in double-muscled cattle as in mice

Antioxidants put Parkinson flies back in the PINK

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