Π-Π Interactions Stabilize PeptoMicelle-Based Formulations of Pretomanid Derivatives Leading to Promising Therapy Against Tuberculosis in Zebrafish and Mouse Models

Dal, Nils-Jørgen Knudsen; Schäfer, Gabriela; Thompson, A. M.; Schmitt, Sascha; Redinger, Natalja; Alonso-Rodriguez, Noelia; Johann, Kerstin; Ojong, Jessica; Wohlmann, Jens; Best, A.; Koynov, Kalonian; Zentel, Rudolph; Shaible, Ulrich E; Griffiths, Gareth; Barz, Matthias; Fenaroli, Federico

doi:10.1101/2022.03.10.483770

Cited by 1 publication

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“…These results most likely stem from the better physical stability of these NPs under dilution conditions and emphasize that TPP crosslinking could be used to control their pharmacokinetics and half‐life time. Considering circulation‐time profiles obtained for other NPs such as those made of poly(γ‐benzyl‐ l ‐glutamic acid)‐ block ‐polysarcosine [ 54 ] or poly(sarcosine)‐ block ‐poly( S ‐ethylsulfonyl)cysteine [ 55 ] that were detected in zebrafish even after 72 h, one could classify the CS‐ g ‐PMMA counterparts as relatively short‐circulating structures.…”

Section: Resultsmentioning

confidence: 99%

Antibiotic‐Loaded Amphiphilic Chitosan Nanoparticles Target Macrophages and Kill an Intracellular Pathogen

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Dal

Fenaroli

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In this work, levofloxacin (LVX), a third‐generation fluoroquinolone antibiotic, is encapsulated within amphiphilic polymeric nanoparticles of a chitosan‐g‐poly(methyl methacrylate) produced by self‐assembly and physically stabilized by ionotropic crosslinking with sodium tripolyphosphate. Non‐crosslinked nanoparticles display a size of 29 nm and a zeta‐potential of +36 mV, while the crosslinked counterparts display 45 nm and +24 mV, respectively. The cell compatibility, uptake, and intracellular trafficking are characterized in the murine alveolar macrophage cell line MH‐S and the human bronchial epithelial cell line BEAS‐2B in vitro. Internalization events are detected after 10 min and the uptake is inhibited by several endocytosis inhibitors, indicating the involvement of complex endocytic pathways. In addition, the nanoparticles are detected in the lysosomal compartment. Then, the antibacterial efficacy of LVX‐loaded nanoformulations (50% w/w drug content) is assessed in MH‐S and BEAS‐2B cells infected with Staphylococcus aureus and the bacterial burden is decreased by 49% and 46%, respectively. In contrast, free LVX leads to a decrease of 8% and 5%, respectively, in the same infected cell lines. Finally, intravenous injection to a zebrafish larval model shows that the nanoparticles accumulate in macrophages and endothelium and demonstrate the promise of these amphiphilic nanoparticles to target intracellular infections.

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Section: Resultsmentioning

confidence: 99%