Immunomimetic Designer Cells Protect Mice from MRSA Infection

  • Ying Liu
  • , Peng Bai
  • , Anne Kathrin Woischnig
  • , Ghislaine Charpin-El Hamri
  • , Haifeng Ye
  • , Marc Folcher
  • , Mingqi Xie
  • , Nina Khanna*
  • , Martin Fussenegger
  • *Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

69 Scopus citations

Abstract

Many community- and hospital-acquired bacterial infections are caused by antibiotic-resistant pathogens. Methicillin-resistant Staphylococcus aureus (MRSA) predisposes humans to invasive infections that are difficult to eradicate. We designed a closed-loop gene network programming mammalian cells to autonomously detect and eliminate bacterial infections. The genetic circuit contains human Toll-like receptors as the bacterial sensor and a synthetic promoter driving reversible and adjustable expression of lysostaphin, a bacteriolytic enzyme highly lethal to S. aureus. Immunomimetic designer cells harboring this genetic circuit exhibited fast and robust sense-and-destroy kinetics against live staphylococci. When tested in a foreign-body infection model in mice, microencapsulated cell implants prevented planktonic MRSA infection and reduced MRSA biofilm formation by 91%. Notably, this system achieved a 100% cure rate of acute MRSA infections, whereas conventional vancomycin treatment failed. These results suggest that immunomimetic designer cells could offer a therapeutic approach for early detection, prevention, and cure of pathogenic infections in the post-antibiotic era. Video Abstract: [Figure presented] Encapsulated mammalian cells with a synthetic gene circuit to sense and respond to MRSA infection could provide potential prophylactic, diagnostic, or therapeutic options for medical implant-associated infections.

Original languageEnglish
Pages (from-to)259-270.e11
JournalCell
Volume174
Issue number2
DOIs
StatePublished - 12 Jul 2018

Keywords

  • Toll-like receptor
  • antibiotic resistance
  • biofilm
  • cell therapy
  • encapsulation
  • implant-associated infection
  • lysostaphin
  • methicillin-resistant Staphylococcus aureus
  • murine tissue cage infection model
  • synthetic gene circuit

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