4.8 Article

Antibacterial Countermeasures via Metal-Organic Framework Supported Sustained Therapeutic Release

Journal

ACS APPLIED MATERIALS & INTERFACES
Volume 11, Issue 8, Pages 7782-7791

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsami.8b21698

Keywords

metal-organic frameworks; drug delivery; therapeutics; ZIF-8; photoluminescence; confocal microscopy

Funding

  1. Laboratory Directed Research Development Program at Sandia National Laboratories
  2. U.S. Department of Energy National Nuclear Security Administration [DE-NA-0003525]

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Long-term antimicrobial therapies are necessary to treat infections caused by virulent intracellular pathogens, including biothreat agents. Current treatment plans include injectable therapeutics given multiple times daily over a period for up to 8 weeks. Here, we present a metal organic framework (MOF), zeolitic imidazolate framework-8 (ZIF-8), as a robust platform to support the sustained release of ceftazidime, an important antimicrobial agent for many critical bacterial infections. Detailed material characterization confirms the successful encapsulation of ceftazidime within the ZIF-8 matrix, indicating sustained drug release for up to a week. The antibacterial properties of ceftazidime@ZIF-8 particles were confirmed against Escherichia coli, chosen here as a representative of Gram-negative bacteria infection model in a proof-of-concept study. Further, we showed that this material system is compatible with macrophage and lung epithelial cell lines, relevant targets for antibacterial therapy for pulmonary and intracellular infections. A promising methodology to enhance the treatment of intracellular infections is to deliver the antibiotic cargo intracellularly. Importantly, this is the first study to unequivocally demonstrate direct MOF particle internalization using confocal microscopy via 3D reconstructions of z-stacks, taking advantage of the intrinsic emission properties of ZIF-8. This is an important development as it circumvents the need to use any staining dyes and addresses current methodology limitations concerning false impression of cargo uptake in the event of the carrier particle breakdown within biological media.

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