Potential allosteric modulators of the proteasome activity

Jankowska, Elżbieta; Gaczyńska, Maria; Osmulski, Paweł A.; Sikorska, Emilia; Rostankowski, R.; Srividya, Madabhushi; Tokmina‐Lukaszewska, Monika; Kasprzykowski, Franciszek

doi:10.1002/bip.21381

Cited by 25 publications

(52 citation statements)

References 45 publications

(87 reference statements)

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“…The diversity of effects exerted on the peptidase activities (i.e., pure noncompetitive inhibition, mixed-type inhibition, or moderate activation) provides the first culprit. We noted similarly diverse effects before with allosteric ligands of the 20S core: PR peptides and peptide fragments of proteins binding to the proteasome (Gaczynska et al, 2003;Jankowska et al, 2010). The AFM-detected rapamycin-induced changes in the dynamics of the gate offer an additional line of evidence for the allosteric nature of rapamycin actions.…”

Section: Discussionmentioning

confidence: 64%

“…4B). Similar to certain other small noncompetitive ligands of the proteasome, the actions of rapamycin were not restricted to inhibition of the peptidases (Jankowska et al, 2010). The T-L peptidase was moderately activated by rapamycin.…”

Section: Resultsmentioning

confidence: 80%

“…A straightforward case of such interference is provided by short peptide sequences derived from C termini of the modules, blocking the grooves and mimicking some allosteric effects of their parent proteins (Jankowska et al, 2010). The anchor peptide fragments of selected regulatory particle ATPases (Rpt) subunits of the 19S, and of PA200 activator, are equipped with the Hb-Y-X motif (hydrophobic amino acid-Tyr-any amino acid) (Ortega et al, 2005;Rabl et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

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Rapamycin Allosterically Inhibits the Proteasome

Osmulski

Gaczyńska

2013

Mol Pharmacol

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Rapamycin is a canonical allosteric inhibitor of the mammalian tarpet of rapamycin (mTOR) kinase with immunosuppressive and proapoptotic activities. We found that in vitro rapamycin also regulates the proteasome, which is an essential intracellular protease of the ubiquitin-proteasome pathway. Rapamycin inhibits proteinase and selected peptidase activities of the catalytic core proteasome at low micromolar concentrations. Moreover, the drug interferes with binding of the 19S cap essential for processing of polyubiquitinylated substrates and with the PA200 proteasome activator to the 20S catalytic core proteasome. These protein complexes are known to bind to specific grooves on the a face region of the 20S core. Treatment with rapamycin affects the conformational dynamics of the proteasomal gate, which is centrally positioned within the a face and allosterically regulated element responsible for the intake of substrates. We showed that rapamycin shares all the proteasome targeting properties not only with other two-domain, closed-ring analogs (rapalogs) but also with its single domain mimics and seco-rapamycin, which is the first in vivo open-ring metabolite of rapamycin that does not affect mTOR. We hypothesize that rapamycin and related compounds bind to the a face and allosterically impact proteasome function. This article discusses the implications of our findings for the mechanism of in vivo actions of rapamycin and for the design of novel allosteric drugs targeting the proteasome.

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Section: Discussionmentioning

confidence: 64%

Section: Resultsmentioning

confidence: 80%

Section: Introductionmentioning

confidence: 99%

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Rapamycin Allosterically Inhibits the Proteasome

Osmulski

Gaczyńska

2013

Mol Pharmacol

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“…The peptide Tat1, comprising residues 48e59 of its parental protein, was proved to be a quite potent noncompetive inhibitor of the human 20S proteasome (h20S). 37 To continue the studies, we synthesized a peptide 16, which was very basic in its character since it consisted mainly of lysine residues, and its mimetic 17 with 3-amino-2,3-dideoxy-a-D-arabino-hexopyranosiduronic acid incorporated in the middle of the sequence (Fig. 10).…”

Section: Hiv Tat-derived Peptidomimetic (17)mentioning

confidence: 99%

Oligomers and peptidomimetics consisting of methyl 3-amino-2,3-dideoxyhexopyranosiduronic acids

et al. 2015

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“…The two 12-residue fragments (Fig. 4C) containing the RTP site and carved out of the basic domain (Tat1), as well as the basic and Gln-rich domains (Tat2) of HIV-1Tat noncompetitively inhibit the ChT-L and PGPH peptidases of the activated human 20S core at high nanomolar concentrations, and also efficiently compete with the core activation by PA28ab complex (65). The Tat1 peptide is better characterized to date than Tat2.…”

Section: Allosteric Route: From the Grooves On A Face To The Gatementioning

confidence: 99%

Harnessing Proteasome Dynamics and Allostery in Drug Design

Gaczyńska

Osmulski

2014

Antioxidants & Redox Signaling

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Significance: The proteasome is the essential protease that is responsible for regulated cleavage of the bulk of intracellular proteins. Its central role in cellular physiology has been exploited in therapies against aggressive cancers where proteasome-specific competitive inhibitors that block proteasome active centers are very effectively used. However, drugs regulating this essential protease are likely to have broader clinical usefulness.

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Potential allosteric modulators of the proteasome activity

Cited by 25 publications

References 45 publications

Rapamycin Allosterically Inhibits the Proteasome

Rapamycin Allosterically Inhibits the Proteasome

Oligomers and peptidomimetics consisting of methyl 3-amino-2,3-dideoxyhexopyranosiduronic acids

Harnessing Proteasome Dynamics and Allostery in Drug Design

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