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Nanomedicine platform for targeting activated neutrophils and neutrophil-platelet complexes using an α 1 -antitrypsin-derived peptide motif.

Michelle A CruzDillon BohincElizabeth A AndraskaJurgis AlvikasShruti RaghunathanNicole A MastersNadine D van KleefKara L BaneKathryn HartKathryn MedrowMichael SunHaitao LiuShannon HaldemanAnkush BanerjeeEmma M LessieurKara HagemanAgharnan GandhiMaria de la FuenteMarvin T NiemanTimothy S KernCoen MaasSteven de MaatKeith B NeevesMatthew D NealAnirban Sen GuptaEvi X Stavrou
Published in: Nature nanotechnology (2022)
Targeted drug delivery to disease-associated activated neutrophils can provide novel therapeutic opportunities while avoiding systemic effects on immune functions. We created a nanomedicine platform that uniquely utilizes an α 1 -antitrypsin-derived peptide to confer binding specificity to neutrophil elastase on activated neutrophils. Surface decoration with this peptide enabled specific anchorage of nanoparticles to activated neutrophils and platelet-neutrophil aggregates, in vitro and in vivo. Nanoparticle delivery of a model drug, hydroxychloroquine, demonstrated significant reduction of neutrophil activities in vitro and a therapeutic effect on murine venous thrombosis in vivo. This innovative approach of cell-specific and activation-state-specific targeting can be applied to several neutrophil-driven pathologies.
Keyphrases
  • cancer therapy
  • drug delivery
  • high throughput
  • single cell
  • emergency department
  • cell therapy
  • binding protein
  • drug release
  • adverse drug