| Literature DB >> 27037901 |
Izidor Sosič1, Martina Gobec1, Boris Brus1, Damijan Knez1, Matej Živec1, Janez Konc2, Samo Lešnik2, Mitja Ogrizek2, Aleš Obreza1, Dušan Žigon3, Dušanka Janežič4, Irena Mlinarič-Raščan1, Stanislav Gobec5.
Abstract
Elevated expression of the immunoproteasome has been associated with autoimmune diseases, inflammatory diseases, and various types of cancer. Selective inhibitors of the immunoproteasome are not only scarce, but also almost entirely restricted to peptide-based compounds. Herein, we describe nonpeptidic reversible inhibitors that selectively block the chymotrypsin-like (β5i) subunit of the human immunoproteasome in the low micromolar range. The most potent of the reversibly acting compounds were then converted into covalent, irreversible, nonpeptidic inhibitors that retained selectivity for the β5i subunit. In addition, these inhibitors discriminate between the immunoproteasome and the constitutive proteasome in cell-based assays. Along with their lack of cytotoxicity, these data point to these nonpeptidic compounds being suitable for further investigation as β5i-selective probes for possible application in noncancer diseases related to the immunoproteasome.Entities:
Keywords: drug design; immunoproteasome; inhibitors; irreversible inhibition; small-molecule inhibitors
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Year: 2016 PMID: 27037901 DOI: 10.1002/anie.201600190
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336