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Hypoxia-inducible lentiviral gene expression in engineered human macrophages.

Harrison K ChinnJennifer L GardellLisa R MatsumotoKevin P LabadieTara N MihailovicNicole A P LiebermanAmira DavisVenu G PillarisettyCourtney A Crane
Published in: Journal for immunotherapy of cancer (2022)
Macrophages engineered to express hypoxia-regulated payloads have the potential to be administered systemically and conditionally express proteins in tissues with hypoxic conditions. In contrast to immune cells that function or survive poorly in hypoxic conditions, macrophages maintain a proinflammatory phenotype that may support continued gene and protein expression when regulated by conditional hypoxia responsive elements and naturally traffic to hypoxic microenvironments, making them ideal vehicles for therapeutic payloads to hypoxic tissues, such as solid tumors. With the ability to fine-tune delivery of potent proteins in response to endogenous microenvironments, macrophage-based cellular therapies may therefore be designed for different disease settings.
Keyphrases
  • gene expression
  • endothelial cells
  • air pollution
  • dna methylation
  • magnetic resonance
  • adipose tissue
  • cancer therapy
  • computed tomography
  • gene therapy
  • anti inflammatory