1. Academic Validation
  2. New 26S proteasome inhibitors with high selectivity for chymotrypsin-like activity and p53-dependent cytotoxicity

New 26S proteasome inhibitors with high selectivity for chymotrypsin-like activity and p53-dependent cytotoxicity

  • ACS Chem Biol. 2013 Feb 15;8(2):353-9. doi: 10.1021/cb300549d.
Paul M Neilsen 1 Ashok D Pehere Kathleen I Pishas David F Callen Andrew D Abell
Affiliations

Affiliation

  • 1 Centre for Personalised Cancer Medicine, Discipline of Medicine, The University of Adelaide, North Terrace, Adelaide SA 5005, Australia.
Abstract

The 26S Proteasome has emerged over the past decade as an attractive therapeutic target in the treatment of cancers. Here, we report new tripeptide aldehydes that are highly specific for the chymotrypsin-like catalytic activity of the Proteasome. These new specific Proteasome inhibitors demonstrated high potency and specificity for sarcoma cells, with therapeutic windows superior to those observed for benchmark Proteasome inhibitors, MG132 and Bortezomib. Constraining the peptide backbone into the β-strand geometry, known to favor binding to a Protease, resulted in decreased activity in vitro and reduced Anticancer activity. Using these new Proteasome inhibitors, we show that the presence of an intact p53 pathway significantly enhances cytotoxic activity, thus suggesting that this tumor suppressor is a critical downstream mediator of cell death following proteasomal inhibition.

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