In vitro and in silico studies of chalcones derived from natural acetophenone inhibitors of NorA and MepA multidrug efflux pumps in Staphylococcus aureus

Thiago S Freitas; Jayze C Xavier; Raimundo L S Pereira; Janaína E Rocha; Fábia F Campina; José B de Araújo Neto; Maria M C Silva; Cristina R S Barbosa; Emmanuel S Marinho; Carlos E S Nogueira; Hélcio S Dos Santos; Henrique D M Coutinho; Alexandre M R Teixeira

doi:10.1016/j.micpath.2021.105286

In vitro and in silico studies of chalcones derived from natural acetophenone inhibitors of NorA and MepA multidrug efflux pumps in Staphylococcus aureus

Microb Pathog. 2021 Dec;161(Pt B):105286. doi: 10.1016/j.micpath.2021.105286. Epub 2021 Nov 16.

Affiliations

¹ Department of Biological Chemistry, Regional University of Cariri, Crato, CE, Brazil.
² Group of Theoretical Chemistry and Electrochemistry, State University of Ceará, Campus FAFIDAM, Limoeiro do Norte, CE, Brazil.
³ Department of Biological Chemistry, Regional University of Cariri, Crato, CE, Brazil; Department of Physics, Regional University of Cariri, Juazeiro do Norte, CE, Brazil.
⁴ Department of Biological Chemistry, Regional University of Cariri, Crato, CE, Brazil; Center for Exact Sciences and Technology - Chemistry Course, Vale do Acaraú University, Sobral, CE, Brazil.
⁵ Department of Biological Chemistry, Regional University of Cariri, Crato, CE, Brazil; Department of Physics, Regional University of Cariri, Juazeiro do Norte, CE, Brazil. Electronic address: alexandre.teixeira@urca.br.

PMID: 34793877
DOI: 10.1016/j.micpath.2021.105286

Abstract

Bacterial resistance induced by efflux pumps is a frequent concern in clinical treatments involving multi-resistant bacteria. Staphylococcus aureus is a microorganism responsible for several types of infections and has several strains carrying efflux pumps, among them are the strain 1199B (NorA overexpresser), and the strain K2068 (MepA overexpresser). In this work, four chalcones derived from Croton anisodontus with modifications in the B ring in their structures were tested regarding their ability to inhibit NorA and MepA efflux pumps. The efflux pump inhibition mechanism was tested with the ethidium bromide substrate in the presence and absence of standard efflux pump inhibitors. The minimum inhibitory concentration values were also compared to those of strains that do not overexpress these efflux pumps. In order to gain some insights about the efflux pump mechanisms of these chalcones, two homology models were created (NorA and MepA) for a docking procedure. In addition, the ADME properties (absorption, distribution, metabolism and excretion) were also evaluated. The tested chalcones promoted synergism of the norfloxacin antibiotic by inhibiting associated efflux pumps. All four tested chalcones appear to bind to the binding sites of the efflux pump models in the same fashion as other chalcones with efflux pump inhibition capabilities. It was also verified that the chalcones 1-4 are well absorbed in the intestine, but with a decrease in their bioavailability, resulting in a low volume of distribution in the blood plasma, in addition to having a mild CNS activity. However, the chalcone 3 and 4 were not toxic due to metabolic activation. Whereas the chalcones 1 and 2 present a mutagenic risk, depending on the oral dose administered. The tested chalcones have not antibacterial activity; however, they are capable of inhibiting efflux pumps for the 1199B and K2068 strains. They promoted synergism of the norfloxacin antibiotic by inhibiting associated efflux pumps, as well as other associated mechanisms.

Keywords: ADMET; Chalcone; Efflux pumps; MepA; Molecular docking; NorA.

MeSH terms

Acetophenones / pharmacology
Anti-Bacterial Agents / pharmacology
Bacterial Proteins / metabolism
Chalcone*
Chalcones* / pharmacology
Microbial Sensitivity Tests
Multidrug Resistance-Associated Proteins
Staphylococcus aureus / metabolism

Substances

Acetophenones
Anti-Bacterial Agents
Bacterial Proteins
Chalcones
Multidrug Resistance-Associated Proteins
Chalcone