Proteasome Activation by Small Molecules

Leestemaker, Yves; Jong, Annemieke de; Witting, Katharina F.; Penning, Renske; Schuurman, Karianne; Rodenko, Boris; Zaal, Esther A.; Kooij, Bert van de; Laufer, Stefan; Heck, Albert J. R.; Borst, Jannie; Scheper, Wiep; Berkers, Celia R.; Ovaa, Huib

doi:10.1016/j.chembiol.2017.05.010

Cited by 119 publications

(111 citation statements)

References 52 publications

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“…We first established that proteasome activity could be modulated in CD8 + T cells with the pan-subunit proteasome inhibitor epoxomicin ( Figure 2A). We then screened a panel of proteasome activators that has been shown to increase proteasome activity in immortalized cell lines (30). Several of these compounds also increased proteasome activity in CD8 + T cells ( Figure 2A).…”

Section: Introductionmentioning

confidence: 99%

“…We observed that cells treated with proteasome inhibitor exhibited an enhanced capacity to produce IFN-γ relative to control-treated cells ( Figure 2C), while one of the proteasome activators we tested (activator 9) reduced cytokine production by CD8 + T cells; we selected this proteasome activator, revealed to be cyclosporine, for subsequent experiments. The activators we tested were identified in a high-throughput screen solely based on their ability to increase proteasome activity (30); thus, they may act through different mechanisms and have unique functional properties. segregation within mitotic CD8 + T cells (11), led us to hypothesize that proteasome activity may be an important regulator of CD8 + T lymphocyte fate specification.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Widjaja¹,

Olvera²,

Metz³

et al. 2017

Journal of Clinical Investigation

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Widjaja¹,

Olvera²,

Metz³

et al. 2017

Journal of Clinical Investigation

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“…Also, there was an accumulation of certain short-lived proteins that normally undergo proteasomal degradation by ubiquitin-dependent (GFPu, UbG767V-GFP) or independent (ODC-GFP) routes (80). Conversely, siRNA-mediated knockdown of endogenous ASK1 enhanced proteasomal peptidase activity and the degradation of these proteins in HEK293 cells, mouse embryonic fibroblasts, and human melanoma cells (80, 82). Thus in these cultures, endogenous ASK1 appears to cause some basal phosphorylation of the 26S proteasome that limits its activity and inhibits intracellular proteolysis.…”

Section: Apoptosis Signal-regulating Kinase 1 (Ask1) and Proteasome Imentioning

confidence: 99%

“…In addition to ASK1, other kinases in the p38 MAPK signaling cascade can repress proteasome function (82, 84). Overexpression of an active mutant of p38 MAPK caused the accumulation of proteins that normally undergo rapid proteasomal degradation by ubiquitin-dependent (GFPu, UbG767V-GFP, Ub-R-GFP) or independent (ODC-GFP) routes (84).…”

Section: Apoptosis Signal-regulating Kinase 1 (Ask1) and Proteasome Imentioning

confidence: 99%

Regulating protein breakdown through proteasome phosphorylation

VerPlank

Goldberg

2017

Biochemical Journal

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The ubiquitin proteasome system degrades the great majority of proteins in mammalian cells. Countless studies have described how ubiquitination promotes the selective degradation of different cell proteins. However, there is a small but growing literature that protein half-lives can also be regulated by post-translational modifications of the 26S proteasome. This article reviews the ability of several kinases to alter proteasome function through subunit phosphorylation. For example, PKA and DYRK2 stimulate the proteasome’s ability to degrade ubiquitinated proteins, peptides, and ATP, while one kinase, ASK1, inhibits proteasome function during apoptosis. Proteasome phosphorylation is likely to be important in regulating protein degradation because it occurs downstream of many hormones and neurotransmitters, in conditions that raise cAMP or cGMP levels, after calcium influx following synaptic depolarization, and during phases of the cell cycle. Beyond its physiological importance, pharmacological manipulation of proteasome phosphorylation has the potential to combat various diseases. Inhibitors of phosphodiesterases by activating PKA or PKG can stimulate proteasomal degradation of misfolded proteins that cause neurodegenerative or myocardial diseases and even reduce the associated pathology in mouse models. These observations are promising since in many proteotoxic diseases, aggregation-prone proteins impair proteasome function and disrupt protein homeostasis. Conversely, preventing subunit phosphorylation by DYRK2 slows cell cycle progression and tumor growth. However, further research is essential to determine how phosphorylation of different subunits by these (or other) kinases alter the properties of this complex molecular machine and thus influence protein degradation rates.

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“…Rolipram inhibits phosphodiesterase 4 thus activating protein kinase A to enhance proteasome activity and in a HD mouse model was shown to alleviate symptoms of neuronal dysfunction 93 . Recently, a series of compounds which enhance proteasome activity were identified using a UPS activity probe 94,95 with p38 MAPK inhibitor PD169316 proving the most potent. Activation of the UPS with these small molecules showed increased proteasome activity and aggregate clearance in a Parkinson's disease model.…”

Section: Therapeutic Approaches In Hd Targeting Upsmentioning

confidence: 99%

Proteostasis in Huntington’s Disease: Disease Mechanisms and Therapeutic Opportunities

Harding

Tong

2018

Preprint

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Abstract:Many neurodegenerative diseases are characterised by impairment of protein quality control mechanisms in neuronal cells. Ineffective clearance of misfolded proteins by the proteasome, autophagy pathways and exocytosis leads to accumulation of toxic protein oligomers and aggregates in neurons.Toxic protein species affect various cellular functions resulting in the development of a spectrum of different neurodegenerative proteinopathies, including Huntington's disease (HD). Playing an integral role in proteostasis, dysfunction of the ubiquitylation system in HD is progressive and multi-faceted with numerous biochemical pathways affected, in particular the ubiquitin proteasome system and autophagy routes for protein aggregate degradation. Unravelling the molecular mechanisms involved in HD pathogenesis of proteostasis provides insight in disease progression in HD as well as possible therapeutic avenues. Recent developments of potential therapeutics are discussed in this review.

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Proteasome Activation by Small Molecules

Cited by 119 publications

References 52 publications

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Regulating protein breakdown through proteasome phosphorylation

Proteostasis in Huntington’s Disease: Disease Mechanisms and Therapeutic Opportunities

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Proteasome Activation by Small Molecules

Cited by 119 publications

References 52 publications

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Proteasome activity regulates CD8+ T lymphocyte metabolism and fate specification

Regulating protein breakdown through proteasome phosphorylation

Proteostasis in Huntington&rsquo;s Disease: Disease Mechanisms and Therapeutic Opportunities

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Product

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Proteostasis in Huntington’s Disease: Disease Mechanisms and Therapeutic Opportunities