Liposomal nanoformulations with trans-caryophyllene and caryophyllene oxide: do they have an inhibitory action on the efflux pumps NorA, Tet(K), MsrA, and MepA?

流出 溴化乙锭 化学 抗生素 抗菌活性 最小抑制浓度 药理学 生物化学 生物 细菌 遗传学 DNA
作者
Jorge Ederson Gonçalves Santana,Cícera Datiane de Morais Oliveira‐Tintino,Gabriel Gonçalves Alencar,Gustavo Miguel Siqueira,José Weverton Almeida‐Bezerra,João Pedro Viana Rodrigues,Vanessa Barbosa Pinheiro Gonçalves,Roberto Nicolete,Saulo Relison Tintino,Henrique Douglas Melo Coutinho,Teresinha Gonçalves da Silva
出处
期刊:Chemico-Biological Interactions [Elsevier BV]
卷期号:393: 110945-110945 被引量:1
标识
DOI:10.1016/j.cbi.2024.110945
摘要

This study aimed to evaluate the antibacterial and inhibitory action of NorA, Tet(K), MsrA and MepA efflux pumps in S. aureus strains using the sesquiterpenes named trans-caryophyllene and caryophyllene oxide, both isolated and encapsulated in liposomes. The antibacterial and inhibitory action of these efflux pumps was evaluated through the serial microdilution test in 96-well microplates. Each sesquiterpene and liposome/sesquiterpene was combined with antibiotics and ethidium bromide (EtBr). The antibiotics named norfloxacin, tetracycline and erythromycin were used. The 1199 B, IS-58, RN4220 and K2068 S. aureus strains carrying NorA, Tet(K), MsrA and MepA, respectively, were tested. In the fluorescence measurement test, K2068 S. aureus was incubated with the sesquiterpenes and EtBr, and the fluorescence emission by EtBr was measured. The tested substances did not show direct antibacterial activity, with MIC >1024 μg/mL. Nonetheless, the isolated trans-caryophyllene and caryophyllene oxide reduced the MIC of antibiotics and EtBr, indicating inhibition of NorA, Tet(K) and MsrA. In the fluorescence test, these same sesquiterpenes increased fluorescence emission, indicating inhibition of MepA. Therefore, the sesquiterpenes named trans-caryophyllene and caryophyllene oxide did not show direct antibacterial action; however, in their isolated form, they showed possible inhibitory action on NorA, Tet(K), MsrA and MepA efflux pumps. They may also act in antibiotic potentiation. Further studies are needed to identify the mechanisms involved in antibiotic potentiation and efflux pump inhibitory action.
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