Stress impact of liposomes loaded with ciprofloxacin on the expression level of MepA and NorB efflux pumps of methicillin-resistant Staphylococcus aureus

One mechanism of ciprofloxacin resistance is attributed to chromosomal DNA-encoded efflux pumps such as the MepA and NorB proteins. The goal of this research is to find a way to bypass Staphylococcus aureus ’ efflux pumps. Because of its high membrane permeability and low association with NorB and M...

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Published in:International microbiology 2022-08, Vol.25 (3), p.427-446
Main Authors: Faraag, Ahmed Hassan Ibrahim, Shafaa, Medhat W., Elkholy, Nourhan S., Abdel-Hafez, Lina Jamil M.
Format: Article
Language:English
Subjects:
Active transport
Antibacterial activity
Antibiotics
Applied Microbiology
Bacteria
Biomedical and Life Sciences
Cell surface
Ciprofloxacin
Deoxyribonucleic acid
DNA
Drug carriers
Drug delivery
Efflux
Encapsulation
Eukaryotic Microbiology
Glycerol
Life Sciences
Liposomes
Medical Microbiology
Membrane permeability
Membranes
Methicillin
Microbial Ecology
Microbiology
Multidrug resistance
NorB protein
Original Article
Permeability
Phosphocholine
Proteins
Pumps
Staphylococcus aureus
Staphylococcus infections
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Summary:One mechanism of ciprofloxacin resistance is attributed to chromosomal DNA-encoded efflux pumps such as the MepA and NorB proteins. The goal of this research is to find a way to bypass Staphylococcus aureus ’ efflux pumps. Because of its high membrane permeability and low association with NorB and MepA efflux proteins, a liposome-encapsulating antibiotic is one of the promising, cost-effective drug carriers and coating mechanisms for overcoming active transport of methicillin-resistant  S. aureus (MRSA) multidrug-resistant efflux protein . The calculated “Log Perm RRCK” membrane permeability values of 1,2-distearoyl-sn-glycerol-3-phosphocholine (DSPC) ciprofloxacin liposome-encapsulated (CFL) showed a lower negative value of − 4,652 cm/s and greater membrane permeability than ciprofloxacin free (CPF). The results of RT-qPCR showed that cationic liposomes containing ciprofloxacin in liposome-encapsulated form (CFL) improved CPF antibacterial activity and affinity for negatively charged bacterial cell surface membrane in comparison to free drug and liposome, as it overcame several resistance mechanisms and reduced the expression of efflux pumps. Ciprofloxacin liposome-encapsulated (CFL) is therefore more effective than ciprofloxacin alone. Liposomes can be combined with a variety of drugs that interact with bacterial cell efflux pumps to maintain high sustained levels of antibiotics in bacterial cells. Graphical abstract
ISSN:1618-1905
1139-6709
1618-1905
DOI:10.1007/s10123-021-00219-4