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Anti-Tumor Immunity Induced by a Ternary Membrane System Derived From Cancer Cells, Dendritic Cells, and Bacteria

  • He Ren
  • , Jiexin Li
  • , Jingyu Zhang
  • , Jingang Liu
  • , Xingyue Yang
  • , Nan Zhang
  • , Qian Qiu
  • , Dan Li
  • , Yue Yu
  • , Xiaofeng Liu
  • , Jonathan F. Lovell
  • , Yumiao Zhang
  • Tianjin University
  • Weifang Medical University
  • Tianjin Medical University

Research output: Contribution to journalArticlepeer-review

17 Scopus citations

Abstract

Cancer vaccines generally are limited by insufficient tumor-specific cellular immunogenicity. Herein, a potent “ABC” ternary membrane-derived vaccine system blended from antigen-presenting mature dendritic cell membranes (“A”), bacterial E. coli cytoplasmic membranes (“B”), and cancer cell membranes (“C”) is developed using a block-copolymer micelle-enabled approach. The respective ABC membrane components provide for a source of cellular immune communication/activation and enhanced accumulation in lymph nodes (A), immunological adjuvant (B), and tumor antigens (C). The introduction of dendritic cell (DC) membranes enables multiple cell-to-cell communication and powerful immune activation. ABC activates dendritic cells and promotes T-cell activation and proliferation in vitro. In vivo, ABC is 14- and 304-fold more immunogenic than binary (BC) and single (C) membrane vaccines, and immunization with ABC enhances the frequency of tumor-specific cytotoxic T lymphocytes, leading to an 80% cure rate in tumor-bearing mice. In a surgical resection and recurrence model, ABC prevents recurrence with vaccination from autologous cancer membranes, and therapeutic effects are observed in a lung metastasis model even with heterologous cancer cell membranes. ABCs formed from human cancer patient-derived tumor cells activate human monocyte-derived dendritic cells (moDC). Taken together, the ternary ABC membrane system provides the needed functional components for personalized cancer immunotherapy.

Original languageEnglish
Article number2302756
JournalSmall
Volume19
Issue number50
DOIs
StatePublished - Dec 13 2023

Keywords

  • biomimetic materials
  • cancer immunotherapy
  • hybrid membrane
  • nanovaccine

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