Screening of the 50000 ChemBridge compound library led to the identification of the oxadiazole-isopropylamide 1 (PI-1833) which inhibited chymotrypsin-like (CT-L) activity (IC50 = 0.60 μM) with little effects on the other two major proteasome proteolytic activities, trypsin-like (T-L) and postglutamyl-peptide-hydrolysis-like (PGPH-L). LC-MS/MS and dialysis show that 1 is a noncovalent and rapidly reversible CT-L inhibitor. Focused library synthesis provided 11ad (PI-1840) with CT-L activity (IC50 = 27 nM). Detailed SAR studies indicate that the amide moiety and the two phenyl rings are sensitive toward modifications. Hydrophobic residues, such as propyl or butyl in the para position (not ortho or meta) of the A-ring and a m-pyridyl group as B-ring, significantly improve activity. Compound 11ad (IC50 = 0.37 μM) is more potent than 1 (IC50 = 3.5 μM) at inhibiting CT-L activity in intact MDA-MB-468 human breast cancer cells and inhibiting their survival. The activity of 11ad warrants further preclinical investigation of this class as noncovalent proteasome inhibitors.
Screening of the 50000 ChemBridge compound library led to the identification of the oxadiazole-isopropylamide 1 (PI-1833) which inhibited n class="Gene">chymotrypsin-like (CT-L) activity (IC50 = 0.60 μM) with little effects on the other two major proteasome proteolytic activities, trypsin-like (T-L) and postglutamyl-peptide-hydrolysis-like (PGPH-L). LC-MS/MS and dialysis show that 1 is a noncovalent and rapidly reversible CT-L inhibitor. Focused library synthesis provided 11ad (PI-1840) with CT-L activity (IC50 = 27 nM). Detailed SAR studies indicate that the amide moiety and the two phenyl rings are sensitive toward modifications. Hydrophobic residues, such as propyl or butyl in the para position (not ortho or meta) of the A-ring and a m-pyridyl group as B-ring, significantly improve activity. Compound 11ad (IC50 = 0.37 μM) is more potent than 1 (IC50 = 3.5 μM) at inhibiting CT-L activity in intact MDA-MB-468humanbreast cancer cells and inhibiting their survival. The activity of 11ad warrants further preclinical investigation of this class as noncovalent proteasome inhibitors.
Authors: Nerea Gallastegui; Philipp Beck; Marcelino Arciniega; Robert Huber; Stefan Hillebrand; Michael Groll Journal: Angew Chem Int Ed Engl Date: 2011-11-21 Impact factor: 15.336
Authors: Christian Perez; Jing Li; Francesco Parlati; Matthieu Rouffet; Yuyong Ma; Andrew L Mackinnon; Tsui-Fen Chou; Raymond J Deshaies; Seth M Cohen Journal: J Med Chem Date: 2017-02-13 Impact factor: 7.446
Authors: Tanner J McDaniel; Theresa A Lansdell; Amila A Dissanayake; Lauren M Azevedo; Jacob Claes; Aaron L Odom; Jetze J Tepe Journal: Bioorg Med Chem Date: 2016-04-02 Impact factor: 3.641
Authors: Bruno O Villoutreix; Melaine A Kuenemann; Jean-Luc Poyet; Heriberto Bruzzoni-Giovanelli; Céline Labbé; David Lagorce; Olivier Sperandio; Maria A Miteva Journal: Mol Inform Date: 2014-06-02 Impact factor: 3.353
Authors: Ruda de Luna Almeida Santos; Lin Bai; Pradeep K Singh; Naoka Murakami; Hao Fan; Wenhu Zhan; Yingrong Zhu; Xiuju Jiang; Kaiming Zhang; Jean Pierre Assker; Carl F Nathan; Huilin Li; Jamil Azzi; Gang Lin Journal: Nat Commun Date: 2017-11-22 Impact factor: 14.919
Authors: Romina A Guedes; Natália Aniceto; Marina A P Andrade; Jorge A R Salvador; Rita C Guedes Journal: Int J Mol Sci Date: 2019-10-25 Impact factor: 5.923