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Combining molecular dynamics and docking simulations of the cytidine deaminase from Mycobacterium tuberculosis H37Rv |
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| Authors: | Luís Fernando Saraiva Macedo Timmers Rodrigo Gay Ducati Zilpa Adriana Sánchez-Quitian Luiz Augusto Basso Diógenes Santiago Santos Walter Filgueira de Azevedo Jr. |
| Affiliation: | 1. Faculdade de Bioci??ncias, Instituto Nacional de Ci??ncia e Tecnologia em Tuberculose (INCT-TB), Laborat??rio de Bioqu??mica Estrutural (LaBioQuest), Pontif??cia Universidade Cat??lica do Rio Grande do Sul (PUCRS), Av. Ipiranga 6681, Porto Alegre, RS, 90619?C900, Brazil 2. Programa de P??s Gradua??o em Biologia Celular e Molecular, Pontif??cia Universidade Cat??lica do Rio Grande do Sul, Porto Alegre, RS, Brazil 3. Centro de Pesquisas em Biologia Molecular e Funcional (CPBMF), Instituto Nacional de Ci??ncia e Tecnologia em Tuberculose (INCT-TB), Pontif??cia Universidade Cat??lica do Rio Grande do Sul (PUCRS), Av. Ipiranga 6681, Porto Alegre, RS, 90619?C900, Brazil |
| Abstract: | Cytidine Deaminase (CD) is an evolutionarily conserved enzyme that participates in the pyrimidine salvage pathway recycling cytidine and deoxycytidine into uridine and deoxyuridine, respectively. Here, our goal is to apply computational techniques in the pursuit of potential inhibitors of Mycobacterium tuberculosis CD (MtCDA) enzyme activity. Molecular docking simulation was applied to find the possible hit compounds. Molecular dynamics simulations were also carried out to investigate the physically relevant motions involved in the protein-ligand recognition process, aiming at providing estimates for free energy of binding. The proposed approach was capable of identifying a potential inhibitor, which was experimentally confirmed by IC50 evaluation. Our findings open up the possibility to extend this protocol to different databases in order to find new potential inhibitors for promising targets based on a rational drug design process. |
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