Nanoparticle Fraught Liposomes: A Platform for Increased Antibiotic Selectivity in Multidrug Resistant Bacteria

Suzan Fangary; Mohammad Abdel-Halim; Reem K Fathalla; Raghda Hassan; Noha Farag; Matthias Engel; Samar Mansour; Salma N Tammam

doi:10.1021/acs.molpharmaceut.2c00258

Nanoparticle Fraught Liposomes: A Platform for Increased Antibiotic Selectivity in Multidrug Resistant Bacteria

Mol Pharm. 2022 Sep 5;19(9):3163-3177. doi: 10.1021/acs.molpharmaceut.2c00258. Epub 2022 Jul 25.

Authors

Suzan Fangary¹, Mohammad Abdel-Halim², Reem K Fathalla³, Raghda Hassan¹, Noha Farag⁴, Matthias Engel³, Samar Mansour^{1

5}, Salma N Tammam¹

Affiliations

¹ Department of Pharmaceutical Technology, German University in Cairo (GUC), New Cairo 11835, Egypt.
² Department of Pharmaceutical Chemistry, German University in Cairo (GUC), New Cairo 24681, Egypt.
³ Pharmaceutical and Medicinal Chemistry, Saarland University, D-66123 Saarbrücken, Germany.
⁴ Department of Microbiology and Immunology, German University in Cairo (GUC), New Cairo 11835, Egypt.
⁵ Department of Pharmaceutics and Industrial Pharmacy-Faculty of Pharmacy, Ain Shams University, Cairo 11566, Egypt.

PMID: 35876358
DOI: 10.1021/acs.molpharmaceut.2c00258

Abstract

Increasing antibiotic concentrations within bacterial cells while reducing them in mammalian ones would ultimately result in an enhancement of antibacterial actions, overcoming multidrug resistance, all while minimizing toxicity. Nanoparticles (NPs) have been used in numerous occasions to overcome antibiotic resistance, poor drug solubility, and stability. However, the concomitant increase in antibiotic concentration in mammalian cells and the resultant toxicity are usually overlooked. Without compromising bacterial cell fusion, large liposomes (Lip) have been reported to show reduced uptake in mammalian cells. Therefore, in this work, small NP fraught liposomes (NP-Lip) were formulated with the aim of increasing NP uptake and antibiotic delivery in bacterial cells but not in mammalian ones. Small polylactic-co-glycolic acid NPs were therefore loaded with erythromycin (Er), an antibiotic with low membrane permeability that is susceptible to drug efflux, and 3c, a 5-cyanothiazolyl urea derivative with low solubility and stability. In vitro experiments demonstrated that the incorporation of small NPs into large Lip resulted in a reduction in NP uptake by HEK293 cells while increasing it in Gram-negative bacteria (Escherichia coli DH5α, E. coli K12, and Pseudomonas aeruginosa), consequently resulting in an enhancement of antibiotic selectivity by fourfold toward E. coli (both strains) and eightfold toward P. aeruginosa. Ocular administration of NP-Lip in a P. aeruginosa keratitis mouse model demonstrated the ability of Er/3c-loaded NP-Lip to result in a complete recovery. More importantly, in comparison to NPs, the ocular administration of NP-Lip showed a reduction in TNF-alpha and IL-6 levels, implying reduced interaction with mammalian cells in vivo. This work therefore clearly demonstrated how tailoring the nano-bio interaction could result in selective drug delivery and a reduction in toxicity.

Keywords: P. aeruginosa keratitis; carbamate derivatives; liposomes; multidrug resistance; nanoparticles; phenyl thiazolyl urea derivatives; selective drug delivery.

MeSH terms

Animals
Anti-Bacterial Agents* / therapeutic use
Drug Resistance, Multiple, Bacterial
Escherichia coli / metabolism
HEK293 Cells
Humans
Liposomes / metabolism
Mammals / metabolism
Mice
Microbial Sensitivity Tests
Nanoparticles*
Pseudomonas aeruginosa

Substances

Anti-Bacterial Agents
Liposomes