Computer-aided Drug Design Investigations for Benzothiazinone Derivatives Against Tuberculosis

Jéssika O Viana; Marcus T Scotti; Luciana Scotti

doi:10.2174/1386207323666200117102316

Computer-aided Drug Design Investigations for Benzothiazinone Derivatives Against Tuberculosis

Comb Chem High Throughput Screen. 2020;23(1):66-82. doi: 10.2174/1386207323666200117102316.

Authors

Jéssika O Viana¹, Marcus T Scotti¹, Luciana Scotti^{1

2}

Affiliations

¹ Federal University of Paraíba, Health Science Center, 50670-910, Joao Pessoa, PB, Brazil.
² Teaching and Research Management, University Hospital, Federal University of Paraíba, João Pessoa, PB, Brazil.

PMID: 31957611
DOI: 10.2174/1386207323666200117102316

Abstract

Background: Tuberculosis (Mycobacterium tuberculosis) is an infectious bacterial disease with the highest levels of mortality worldwide, presenting numerous cases of resistance. In silico studies, which elaborate chemical and biological models in computational tools and make it possible to interpret molecular characteristics, are among the methods used in the search for new drugs.

Objective: In this perspective, our aim was to use QSAR and molecular modeling to propose possible pharmacophores from benzothiazinone derivatives.

Methods: In this study, a set of 69 benzothiazinone derivatives, together with computational tools such as molecular descriptor analysis in chemometrics, metabolic prediction, and molecular coupling to 4 proteins: DprE1, InhA, PS, and DHFR important for the bacillus were investigated.

Results: The chemometric model computed in the Volsurf+ program presented good predictive values for both amphiphilicity and molecular volume. These are essential for biological activity. Metabolites from the cytochrome isoforms CYP3A4 and 2D6 interactions revealed coupling divergences which, noting that the metabolites did not present changes to the QSAR proposed pharmacophore structures, may be due to the reaction medium and existing differences in the benzothiazinone structures. Similarly, molecular docking with the four TB enzymes presented good interactions for the more active compounds. The fragments found using QSAR (being essential for biological activity) also presented as being essential for ligand-protein site interactions.

Conclusion: From the benzothiazinone derivative series evaluated, compound 11026134 presented the best profile in all study analyses, noting that the trifluoromethyl, nitro group, and piperazine fragment with aliphatic hydrocarbon groups are likely pharmacophores for the benzothiazinones studied.

Keywords: Antitubercular drugs; QSAR; benzothiazinones; metabolic prediction; molecular docking; pharmacophore..

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antitubercular Agents / chemical synthesis
Antitubercular Agents / chemistry
Antitubercular Agents / therapeutic use*
Computer-Aided Design*
Drug Design*
Microbial Sensitivity Tests
Molecular Structure
Mycobacterium tuberculosis / drug effects*
Thiazines / chemical synthesis
Thiazines / chemistry
Thiazines / therapeutic use*
Tuberculosis / drug therapy*

Substances

Antitubercular Agents
Thiazines