| Literature DB >> 34095840 |
Vinicius Bonatto1, Pedro Henrique Jatai Batista1, Lorenzo Cianni1, Daniela De Vita1, Daniel G Silva1, Rodrigo Cedron1, Daiane Y Tezuka1,2, Sérgio de Albuquerque2, Carolina Borsoi Moraes3, Caio Haddad Franco3, Jerônimo Lameira1,4, Andrei Leitão1, Carlos A Montanari1.
Abstract
The cysteine protease cruzipain is considered to be a validated target for therapeutic intervention in the treatment of Chagas disease. Hence, peptidomimetic cruzipain inhibitors having a reactive group (known as warhead) are subject to continuous studies to discover novel antichagasic compounds. Here, we evaluated how different warheads for a set of structurally similar related compounds could inhibit the activity of cruzipain and, ultimately, their trypanocidal effect. We first investigated in silico the intrinsic reactivity of these compounds by applying the Fukui index to correlate it with the enzymatic affinity. Then, we evaluated their potency against T. cruzi (Y and Tulahuen strains), which revealed the reversible cruzain inhibitor Neq0656 as a better trypanocidal agent (ECY.strain 50 = 0.1 μM; SI = 58.4) than the current drug benznidazole (ECY.strain 50 = 5.1 μM; SI > 19.6). We also measured the half-life time by HPLC analysis of three lead compounds in the presence of glutathione and cysteine to experimentally assess their intrinsic reactivity. Results clearly illustrated the reactivity trend for the warheads (azanitrile > aldehyde > nitrile), where the aldehyde displayed an intermediate intrinsic reactivity. Therefore, the aldehyde bearing peptidomimetic compounds should be subject for in-depth evaluation in the drug discovery process. This journal is © The Royal Society of Chemistry.Entities:
Year: 2020 PMID: 34095840 PMCID: PMC8126975 DOI: 10.1039/d0md00097c
Source DB: PubMed Journal: RSC Med Chem ISSN: 2632-8682