Overcoming Therapeutic Challenges of Antibiotic Delivery with Cubosome Lipid Nanocarriers.
Brendan P DyettSampa SarkarHaitao YuJamie StrachanCalum John DrummondCharlotte E ConnPublished in: ACS applied materials & interfaces (2024)
Low discovery rates for new antibiotics, commercial disincentives to invest, and inappropriate use of existing drugs have created a perfect storm of antimicrobial resistance (AMR). This "silent pandemic" of AMR looms as an immense, global threat to human health. In tandem, many potential novel drug candidates are not progressed due to elevated hydrophobicity, which may result in poor intracellular internalization and undesirable serum protein binding. With a reducing arsenal of effective antibiotics, enabling technology platforms that improve the outcome of treatments, such as repurposing existing bioactive agents, is a prospective option. Nanocarrier (NC) mediated drug delivery is one avenue for amplifying the therapeutic outcome. Here, the performance of several antibiotic classes encapsulated within the lipid-based cubosomes is examined. The findings demonstrate that encapsulation affords significant improvements in drug concentration:inhibition outcomes and assists in other therapeutic challenges associated with internalization, enzyme degradation, and protein binding. We emphasize that a currently sidelined compound, novobiocin, became active and revealed a significant increase in inhibition against the pathogenic Gram-negative strain, Pseudomonas aeruginosa . Encapsulation affords co-delivery of multiple bioactives as a strategy for mitigating failure of monotherapies and tackling resistance. The rationale in optimized drug selection and nanocarrier choice is examined by transport modeling which agrees with experimental inhibition results. The results demonstrate that lipid nanocarrier encapsulation may alleviate a range of challenges faced by antibiotic therapies and increase the range of antibiotics available to treat bacterial infections.
Keyphrases
- drug delivery
- antimicrobial resistance
- human health
- gram negative
- pseudomonas aeruginosa
- cancer therapy
- risk assessment
- multidrug resistant
- binding protein
- drug release
- fatty acid
- sars cov
- protein protein
- small molecule
- drug induced
- cystic fibrosis
- coronavirus disease
- single cell
- climate change
- acinetobacter baumannii
- escherichia coli
- biofilm formation
- dna binding
- amino acid
- reactive oxygen species