Towards an arthritis flare-responsive drug delivery system.
Nitin JoshiJing YanSeth LevySachin BhagchandaniKai V SlaughterNicholas E ShermanJulian AmiraultYufeng WangLogan RiegelXueyin HeTan Shi RuiMichael ValicPraveen K VemulaOscar R MirandaOren LevyEllen M GravalleseAntonios O AliprantisJoerg ErmannJeffrey M KarpPublished in: Nature communications (2018)
Local delivery of therapeutics for the treatment of inflammatory arthritis (IA) is limited by short intra-articular half-lives. Since IA severity often fluctuates over time, a local drug delivery method that titrates drug release to arthritis activity would represent an attractive paradigm in IA therapy. Here we report the development of a hydrogel platform that exhibits disassembly and drug release controlled by the concentration of enzymes expressed during arthritis flares. In vitro, hydrogel loaded with triamcinolone acetonide (TA) releases drug on-demand upon exposure to enzymes or synovial fluid from patients with rheumatoid arthritis. In arthritic mice, hydrogel loaded with a fluorescent dye demonstrates flare-dependent disassembly measured as loss of fluorescence. Moreover, a single dose of TA-loaded hydrogel but not the equivalent dose of locally injected free TA reduces arthritis activity in the injected paw. Together, our data suggest flare-responsive hydrogel as a promising next-generation drug delivery approach for the treatment of IA.
Keyphrases
- drug delivery
- drug release
- cancer therapy
- rheumatoid arthritis
- oxidative stress
- small molecule
- emergency department
- stem cells
- combination therapy
- high throughput
- big data
- quantum dots
- type diabetes
- machine learning
- insulin resistance
- skeletal muscle
- adipose tissue
- replacement therapy
- artificial intelligence
- cell therapy
- aqueous solution