AI Article Synopsis

  • The study investigates a new method for treating osteoarthritis by using a polyurethane polymer linked to the anti-inflammatory drug diclofenac for direct injection into joints.
  • The polymer allows for controlled drug release, effectively delivering medication over a 15-day period, which may minimize common side effects associated with oral NSAIDs.
  • Animal testing showed that the polymer remains in the joints for an extended time and significantly reduces pain and inflammation, highlighting its potential for long-term osteoarthritis treatment.

Article Abstract

The most common treatment for osteoarthritis is daily oral administration of a nonsteroidal anti-inflammatory drug such as diclofenac. This daily dosage regime is often associated with severe side effects. In this study, we explored the potential of utilizing a high molecular weight cross-linked polyurethane polymer covalently linked to diclofenac () for intra-articular administration. We aim to exploit the advantages of local drug delivery by developing an implant with improved efficacy and reduced side effects. The polymer was synthesized from a diclofenac-functionalized monomer unit in a simple one-pot reaction, followed by cross-linking. drug release studies showed zero-order drug release for 4 days, followed by a gradual decline in drug release rate until diclofenac was depleted after 15 days. The cross-linked polymer was triturated to yield an injectable microgel formulation for administration. Whole animal fluorescence imaging of the rhodamine-labeled showed good retention of the polymer in the knee joints of healthy rats, with approximately 30% of the injected dose still present 2 weeks post intra-articular administration. In a reactivation arthritis animal model, the formulation reduced pain and significantly reduced inflammation after a short lag phase, showing that this drug delivery system warrants further development for long-term treatment of osteoarthritis with the benefit of reduced side effects.

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Source
http://dx.doi.org/10.1021/acsabm.9b00232DOI Listing

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