Dual role of
            <scp>USP</scp>
            30 in controlling basal pexophagy and mitophagy

Marcassa, Elena; Kallinos, Andreas; Jardine, Jane; Rusilowicz‐Jones, Emma V; Amador, Martínez; Kuehl, Sandra; Islinger, Markus; Clague, Michael J.; Urbé, Sylvie

doi:10.15252/embr.201745595

Cited by 125 publications

(181 citation statements)

References 48 publications

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“…We see enhanced pUb accumulation in the absence of USP30 activity, despite the published observations that pUb modified chains provide a poor substrate for USP30 (9,41). How then might USP30 suppress mitophagy, as previously reported in several studies (20,(22)(23)(24)? We have previously shown that USP30 depletion enhances PINK1-dependent basal mitophagy even in the absence of Parkin (20).…”

Section: Discussioncontrasting

confidence: 45%

“…USP30 is one of only two DUBs that possess a transmembrane domain. Its localisation is restricted to the outer mitochondrial membrane and to peroxisomes (18)(19)(20)(21). USP30 can limit the Parkin-dependent ubiquitylation of selected substrates and depolarisation-induced mitophagy in cell systems that have been engineered to over-express Parkin (22)(23)(24)(25).…”

Section: Introductionmentioning

confidence: 99%

“…USP30 can limit the Parkin-dependent ubiquitylation of selected substrates and depolarisation-induced mitophagy in cell systems that have been engineered to over-express Parkin (22)(23)(24)(25). We have recently shown that it can also suppress a PINK1-dependent component of basal mitophagy, even in cells that do not express Parkin (20). Thus USP30 may represent an actionable drug target relevant to PD progression and other pathologies to which defective mitophagy can contribute (26)(27)(28).…”

Section: Introductionmentioning

confidence: 99%

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A novel USP30 inhibitor recapitulates genetic loss of USP30 and sets the trigger for PINK1-PARKIN amplification of mitochondrial ubiquitylation

Rusilowicz‐Jones

Jardine

Pinto-Fernández

et al. 2020

Preprint

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The mitochondrial deubiquitylase USP30 negatively regulates the selective autophagy of damaged mitochondria. It has been proposed as an actionable target to alleviate the loss of function of the mitophagy pathway governed by the Parkinson's Disease associated genes PINK1 and PRKN. We present the characterisation of a N-cyano pyrrolidine derived compound, FT3967385, with high selectivity for USP30. The compound is well tolerated with no loss of total mitochondrial mass. We demonstrate that ubiquitylation of TOM20, a component of the outer mitochondrial membrane import machinery that directly interacts with USP30, represents a robust biomarker for both USP30 loss and inhibition. We have conducted proteomics analyses on a SHSY5Y neuroblastoma cell line model to directly compare the effects of genetic loss of USP30 with selective inhibition in an unbiased fashion. We have thereby identified a subset of ubiquitylation events consequent to mitochondrial depolarisation that are USP30 sensitive. Within responsive elements of the ubiquitylome, several components of the outer mitochondrial membrane transport (TOM) complex are most prominent. Thus, our data support a model whereby USP30 can regulate the availability of ubiquitin at the specific site of mitochondrial PINK1 accumulation following membrane depolarisation. In this model, USP30 deubiquitylation of TOM complex components dampens the trigger for the Parkin-dependent amplification of mitochondrial ubiquitylation leading to mitophagy. Accordingly, PINK1 generation of phospho-Ser65 Ubiquitin proceeds more rapidly and to a greater extent in cells either lacking USP30 or subject to USP30 inhibition.

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Section: Discussioncontrasting

confidence: 45%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A novel USP30 inhibitor recapitulates genetic loss of USP30 and sets the trigger for PINK1-PARKIN amplification of mitochondrial ubiquitylation

Rusilowicz‐Jones

Jardine

Pinto-Fernández

et al. 2020

Preprint

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“…Interestingly, Cichocki et al [63] also show that the loss of Pex19 impinges upon mitochondrial targeting. Consequently, the ability to control the extent of the mitochondrial and peroxisomal localisation of Miro may be an important regulatory axis; an axis that likely includes members of an ever-growing list of proteins targeted to both organelles including USP30, Fis1, Mff, MUL1/MAPL, OMP25, BCL-XL, BCL-2, MAVS and GDAP1 [8,10,[21][22][23][24][25]. With this in mind, we propose the following model: the Miro transmembrane domain is required for Pex19 binding and peroxisomal localisation of Miro.…”

Section: Discussionmentioning

confidence: 99%

“…These include Fis1, Mff, Drp1, GDAP1, USP30, MUL1/MAPL, OMP25, MAVS, BCL-XL, BCL-2 and more recently Miro1/2 [6,10,[21][22][23][24][25][26]. These include Fis1, Mff, Drp1, GDAP1, USP30, MUL1/MAPL, OMP25, MAVS, BCL-XL, BCL-2 and more recently Miro1/2 [6,10,[21][22][23][24][25][26].…”

Section: Introductionmentioning

confidence: 99%

Peroxisomal fission is modulated by the mitochondrial Rho‐GTPases, Miro1 and Miro2

et al. 2020

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Peroxisomes are essential for a number of cellular functions, including reactive oxygen species metabolism, fatty acid b-oxidation and lipid synthesis. To ensure optimal functionality, peroxisomal size, shape and number must be dynamically maintained; however, many aspects of how this is regulated remain poorly characterised. Here, we show that the localisation of Miro1 and Miro2-outer mitochondrial membrane proteins essential for mitochondrial trafficking-to peroxisomes is not required for basal peroxisomal distribution and long-range trafficking, but rather for the maintenance of peroxisomal size and morphology through peroxisomal fission. Mechanistically, this is achieved by Miro negatively regulating Drp1-dependent fission, a function that is shared with the mitochondria. We further find that the peroxisomal localisation of Miro is regulated by its first GTPase domain and is mediated by an interaction through its transmembrane domain with the peroxisomal-membrane protein chaperone, Pex19. Our work highlights a shared regulatory role of Miro in maintaining the morphology of both peroxisomes and mitochondria, supporting a crosstalk between peroxisomal and mitochondrial biology.

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The PINK1 repertoire: Not just a one trick pony

et al. 2021

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PTEN-induced kinase 1 (PINK1) is a Parkinson's disease gene that acts as a sensor for mitochondrial damage. Its best understood role involves phosphorylating ubiquitin and the E3 ligase Parkin (PRKN) to trigger a ubiquitylation cascade that results in selective clearance of damaged mitochondria through mitophagy. Here we focus on other physiological roles of PINK1. Some of these also lie upstream of Parkin but others represent autonomous functions, for which alternative substrates have been identified.We argue that PINK1 orchestrates a multi-arm response to mitochondrial damage that impacts on mitochondrial architecture and biogenesis, calcium handling, transcription and translation. We further discuss a role for PINK1 in immune signalling co-ordinated at mitochondria and consider the significance of a freely diffusible cleavage product, that is constitutively generated and degraded under basal conditions.

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Dual role of USP 30 in controlling basal pexophagy and mitophagy

Cited by 125 publications

References 48 publications

A novel USP30 inhibitor recapitulates genetic loss of USP30 and sets the trigger for PINK1-PARKIN amplification of mitochondrial ubiquitylation

A novel USP30 inhibitor recapitulates genetic loss of USP30 and sets the trigger for PINK1-PARKIN amplification of mitochondrial ubiquitylation

Peroxisomal fission is modulated by the mitochondrial Rho‐GTPases, Miro1 and Miro2

The PINK1 repertoire: Not just a one trick pony

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