Development of Novel Selective Peptidomimetics Containing a Boronic Acid Moiety, Targeting the 20S Proteasome as Anticancer Agents

Scarbaci, Kety; Troiano, Valeria; Ettari, Roberta; Pinto, Andrea; Micale, Nicola; Giovanni, Carmen Di; Cerchia, Carmen; Schirmeister, Tanja; Novellino, Ettore; Lavecchia, Antonio; Zappalà, Maria; Grasso, Silvana

doi:10.1002/cmdc.201402075

Cited by 13 publications

(6 citation statements)

References 44 publications

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“…Splitting patterns are described as singlet (s), broad singlet (br s), doublet (d), triplet (t), quartet (q), multiplet (m), doublet of doublets (dd), doublet of doublets of doublets (ddd), or triplet of doublets (td). Compounds 27 – 30 were synthesized as previously reported …”

Section: Methodsmentioning

confidence: 99%

“…In this context, our research group has been actively involved in the development of novel 20S proteasome inhibitors . In particular, we have identified a series of amides, some of which were active against the chymotrypsin‐like activity of the 20S proteasome with K i values in the sub‐micromolar range. The noncovalent binding mode of the most active inhibitors was corroborated by docking simulations into the crystal structure of the yeast 20S proteasome.…”

Section: Introductionmentioning

confidence: 99%

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Development of Novel Amides as Noncovalent Inhibitors of Immunoproteasomes

et al. 2019

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The development of immunoproteasome‐selective inhibitors is a promising strategy for treating hematologic malignancies, autoimmune and inflammatory diseases. In this context, we report the design, synthesis, and biological evaluation of a new series of amide derivatives as immunoproteasome inhibitors. Notably, the designed compounds act as noncovalent inhibitors, which might be a promising therapeutic option because of the lack of drawbacks and side effects associated with irreversible inhibition. Among the synthesized compounds, we identified a panel of active inhibitors with Ki values in the low micromolar or sub‐micromolar ranges toward the β5i and/or β1i subunits of immunoproteasomes. One of the active compounds was shown to be the most potent and selective inhibitor with a Ki value of 21 nm against the single β1i subunit. Docking studies allowed us to determine the mode of binding of the molecules in the catalytic site of immunoproteasome subunits.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Development of Novel Amides as Noncovalent Inhibitors of Immunoproteasomes

et al. 2019

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“…Docking results predicted promising activities as PIs ( Table 1 ). With these results in hand, we decided to evaluate the in vitro inhibitory activity of compounds 15 – 25 against the ChT-L activity of the human 20S proteasome [ 31 , 44 , 62 , 63 , 64 , 65 , 66 ]. The calculated free energies of binding (Δ G ) and the calculated and experimental Ki values at the binding site of the proteasome are reported in Table 1 .…”

Section: Resultsmentioning

confidence: 99%

Novel Class of Proteasome Inhibitors: In Silico and In Vitro Evaluation of Diverse Chloro(trifluoromethyl)aziridines

Ielo

Patamia

Citarella

et al. 2022

IJMS

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The ubiquitin-proteasome pathway (UPP) is the major proteolytic system in the cytosol and nucleus of all eukaryotic cells. The role of proteasome inhibitors (PIs) as critical agents for regulating cancer cell death has been established. Aziridine derivatives are well-known alkylating agents employed against cancer. However, to the best of our knowledge, aziridine derivatives showing inhibitory activity towards proteasome have never been described before. Herein we report a new class of selective and nonPIs bearing an aziridine ring as a core structure. In vitro cell-based assays (two leukemia cell lines) also displayed anti-proliferative activity for some compounds. In silico studies indicated non-covalent binding mode and drug-likeness for these derivatives. Taken together, these results are promising for developing more potent PIs.

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“…The biological evaluation of the compounds in the human 20S proteasome showed a promising inhibition profile, mainly for compounds bearing a P2 ethylene fragment ( K i values in the nM range for the CT-L active site). Docking experiments into the yeast 20S proteasome were performed according to a protocol previously applied by the same group [146] and showed that the ligands are accommodated mostly into the CT-L site, establishing a covalent bond with the catalytic Thr1 via the boron atom [145].…”

Section: Computer-aided Drug Designmentioning

confidence: 99%

Computational Approaches for the Discovery of Human Proteasome Inhibitors: An Overview

et al. 2016

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Abstract:Proteasome emerged as an important target in recent pharmacological research due to its pivotal role in degrading proteins in the cytoplasm and nucleus of eukaryotic cells, regulating a wide variety of cellular pathways, including cell growth and proliferation, apoptosis, DNA repair, transcription, immune response, and signaling processes. The last two decades witnessed intensive efforts to discover 20S proteasome inhibitors with significant chemical diversity and efficacy. To date, the US FDA approved to market three proteasome inhibitors: bortezomib, carfilzomib, and ixazomib. However new, safer and more efficient drugs are still required. Computer-aided drug discovery has long being used in drug discovery campaigns targeting the human proteasome. The aim of this review is to illustrate selected in silico methods like homology modeling, molecular docking, pharmacophore modeling, virtual screening, and combined methods that have been used in proteasome inhibitors discovery. Applications of these methods to proteasome inhibitors discovery will also be presented and discussed to raise improvements in this particular field.

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Development of Novel Selective Peptidomimetics Containing a Boronic Acid Moiety, Targeting the 20S Proteasome as Anticancer Agents

Cited by 13 publications

References 44 publications

Development of Novel Amides as Noncovalent Inhibitors of Immunoproteasomes

Development of Novel Amides as Noncovalent Inhibitors of Immunoproteasomes

Novel Class of Proteasome Inhibitors: In Silico and In Vitro Evaluation of Diverse Chloro(trifluoromethyl)aziridines

Computational Approaches for the Discovery of Human Proteasome Inhibitors: An Overview

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