Vps35 Mediates Vesicle Transport between the Mitochondria and Peroxisomes

Braschi, Emélie; Goyon, Vanessa; Zunino, Rodolfo; Mohanty, Abhishek; Xu, Liqun; McBride, Heidi M.

doi:10.1016/j.cub.2010.05.066

Cited by 260 publications

(249 citation statements)

References 32 publications

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“…However, the effects of nocodazole treatment in the present study indicate that microtubule polymerization is required for the translocation of FKBP38 from the mitochondria to the ER. Vesicle transport occurs between various organelles, with such communication having recently been shown to take place between the mitochondria and both peroxisomes and lysosomes 46,47 . Small vesicles might thus be generated as a consequence of mitochondrial membrane damage and then be transported to the ER by the microtubule-dependent trafficking system.…”

Section: Discussionmentioning

confidence: 99%

Selective escape of proteins from the mitochondria during mitophagy

2013

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Mitophagy refers to the degradation of mitochondria by the autophagy system that is regulated by Parkin and PINK1, mutations in the genes for which have been linked to Parkinson's disease. Here we show that certain mitochondrial outer membrane proteins, including FKBP38 and Bcl-2, translocate from the mitochondria to the endoplasmic reticulum (ER) during mitophagy, thereby escaping degradation by autophagosomes. This translocation depends on the ubiquitylation activity of Parkin and on microtubule polymerization. Photoconversion analysis confirmed that FKBP38 detected at the ER during mitophagy indeed represents preexisting protein transported from the mitochondria. The escape of FKBP38 and Bcl-2 from the mitochondria is determined by the number of basic amino acids in their COOH-terminal signal sequences. Furthermore, the translocation of FKBP38 is essential for the suppression of apoptosis during mitophagy. Our results thus show that not all mitochondrial proteins are degraded during mitophagy, with some proteins being evacuated to the ER to prevent unwanted apoptosis.

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Section: Discussionmentioning

confidence: 99%

Selective escape of proteins from the mitochondria during mitophagy

2013

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“…The D620N PD-related mutation in VPS35 displays a dominant negative missorting phenotype of retrograde transport of proteins dependent on the WASH complex [218,222]. WT VPS35 regulates mitochondrial-anchored protein ligase transport from the mitochondria to the peroxisomes [223], suggesting that VPS35 mutations may produce mitochondrial defects in patients. VPS35 is also responsible for divalent metal transporter 1 transport [224].…”

Section: Vps35 (Park17)mentioning

confidence: 99%

Neural stem cells in Parkinson’s disease: a role for neurogenesis defects in onset and progression

Grand

Gonzalez-Cano

Pavlou

et al. 2014

Cell. Mol. Life Sci.

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Parkinson's disease (PD) is the second most common neurodegenerative disorder, leading to a variety of motor and non-motor symptoms. Interestingly, nonmotor symptoms often appear a decade or more before the first signs of motor symptoms. Some of these non-motor symptoms are remarkably similar to those observed in cases of impaired neurogenesis and several PD-related genes have been shown to play a role in embryonic or adult neurogenesis. Indeed, animal models deficient in Nurr1, Pitx3, SNCA and PINK1 display deregulated embryonic neurogenesis and LRRK2 and VPS35 have been implicated in neuronal development-related processes such as Wnt/bcatenin signaling and neurite outgrowth. Moreover, adult neurogenesis is affected in both PD patients and PD animal models and is regulated by dopamine and dopaminergic (DA) receptors, by chronic neuroinflammation, such as that observed in PD, and by differential expression of wild-type or mutant forms of PD-related genes. Indeed, an increasing number of in vivo studies demonstrate a role for SNCA and LRRK2 in adult neurogenesis and in the generation and maintenance of DA neurons. Finally, the roles of PDrelated genes, SNCA, LRRK2, VPS35, Parkin, PINK1 and DJ-1 have been studied in NSCs, progenitor cells and induced pluripotent stem cells, demonstrating a role for some of these genes in stem/progenitor cell proliferation and maintenance. Together, these studies strongly suggest a link between deregulated neurogenesis and the onset and progression of PD and present strong evidence that, in addition to a neurodegenerative disorder, PD can also be regarded as a developmental disorder.

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“…[33][34][35][36] Recently an export system that transfers proteins from mitochondria to peroxisomes via vesicular trafficking has also been identified. 37 These dynamic properties of mitochondria mean that the mitochondrial proteome is not static, but varies with cell type and state.…”

Section: Introductionmentioning

confidence: 99%