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Targeted Protein Degradation Mediated by Genetically Engineered Lysosome-Targeting Exosomes.

Tao WangLiang SunTianyu RenMin HouYing LongJian-Hui JiangJianjun He
Published in: Nano letters (2023)
Protein-degrading chimeras are superior drug modalities compared to traditional protein inhibitors because of their effective therapeutic performance. So far, various targeted protein degradation strategies, including proteolysis-targeting chimeras and lysosome-targeting chimeras, have emerged as essential technologies for tackling diseases caused by abnormal protein expression. Here, we report the development and application of lysosome-targeting exosomes (LYTEXs) for the selective degradation of membrane protein targets. LYTEXs are genetically engineered exosomes expressing multivalent single-chain fragment variables, simultaneously recognizing cell-surface lysosome-targeting and to-be-degraded protein. We show that by targeting the lysosome-directing asialoglycoprotein receptor, bispecific LYTEXs can induce lysosomal degradation of membrane-associated therapeutic targets. This strategy provides a generalizable, easy-to-prepare platform for modulating surface protein expression, with the advantage of therapeutic delivery.
Keyphrases
  • cancer therapy
  • protein protein
  • fluorescent probe
  • mesenchymal stem cells
  • stem cells
  • living cells
  • binding protein
  • amino acid
  • emergency department
  • cell surface
  • drug delivery
  • small molecule