P4 and P1' Optimization of Bicycloproline P2 Bearing Tetrapeptidyl Alpha-ketoamides As HCV Protease Inhibitors
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With the aim of improving HCV protease inhibitors reported in our previous manuscripts, we synthesized and evaluated a series of 1a-based tetrapeptidyl alpha-ketoamides with additional P4 modification. The promising analog discovered through this SAR, 5a, was further derivatized at P1' or P1 position. As a result of these efforts, we found that replacement of the P4 valine as seen in 1a with cyclohexylglycine (Chg) resulted in the discovery of 5a, 5c, and 5e endowed with improved cellular activity in comparison to 1a.
Iman K, Mirza M, Sadia F, Froeyen M, Trant J, Chaudhary S Viruses. 2024; 16(8).
PMID: 39205224 PMC: 11359326. DOI: 10.3390/v16081250.
Chen X, Huang X, Ma Q, Kuzmic P, Zhou B, Zhang S Nat Microbiol. 2024; 9(4):1075-1088.
PMID: 38553607 PMC: 10994847. DOI: 10.1038/s41564-024-01618-9.
Modern Multicomponent Reactions for better Drug Syntheses**.
Zarganes-Tzitzikas T, Domling A Org Chem Front. 2014; 1(7):834-837.
PMID: 25147729 PMC: 4136525. DOI: 10.1039/C4QO00088A.
White P, Llinas-Brunet M, Amad M, Bethell R, Bolger G, Cordingley M Antimicrob Agents Chemother. 2010; 54(11):4611-8.
PMID: 20823284 PMC: 2976164. DOI: 10.1128/AAC.00787-10.
Substituted imidazopyridines as potent inhibitors of HCV replication.
Vliegen I, Paeshuyse J, De Burghgraeve T, Lehman L, Paulson M, Shih I J Hepatol. 2009; 50(5):999-1009.
PMID: 19303654 PMC: 7114863. DOI: 10.1016/j.jhep.2008.12.028.