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Spleen-tumor dual-targeting vaccines reshape anticancer landscape by activating both innate and adaptive immunity

  • Wenfei Xu
  • , Xiaoyan Li
  • , Wenqiang Hu
  • , Jiaxin Zhou
  • , Xing Liu
  • , Jianbo Yu
  • , Fan Zhang*
  • , Weidong Nie*
  • , Guihong Lu*
  • , Yanli Zhao*
  • *此作品的通讯作者
  • Shenzhen Children's Hospital
  • Beijing Institute of Technology
  • Longgang Central Hospital
  • Nanyang Technological University
  • Institute of Biomedical Engineering, Chinese Academy of Medical Sciences and Peking Union Medical College

科研成果: 期刊稿件文章同行评审

摘要

Owing to the reticular structure and dense lymphocyte concentration within the spleen, spleen-targeted vaccines can overcome the challenges faced by conventional vaccines, such as inefficient antigen delivery and delayed immune activation. However, the existing spleen-targeted vaccines are ineffective in preventing and treating immunologically cold tumors. Herein, we develop a spleen/tumor dual-target hybrid vaccine that combines red blood cell membrane-derived vesicles (RBCVs) and bacterial outer membrane vesicles (OMVs) to deliver tumor antigens. This hybrid vaccine utilizes RBCVs to enhance the biosafety of OMVs and endows them with a spleen-targeting ability. Co-delivery of OMVs as adjuvants with tumor antigens to the spleen triggers rapid and robust immune responses, promoting immune memory formation to prevent the development and metastasis of immunologically cold tumors. In addition to acting as vaccine adjuvants, OMVs can target and remodel the immunosuppressive tumor microenvironment by reprogramming tumor-associated macrophages and downregulating regulatory T cells, thereby enhancing the immune responses induced by vaccines and immune checkpoint inhibitors. Because of their antigen-loading flexibility, these versatile vesicles can be used for the spleen-targeted delivery of various protein- or nucleic acid-based antigens, offering a safe and promising strategy for the prevention and treatment of diverse tumors and pathogens.

源语言英语
文章编号124279
期刊Biomaterials
334
DOI
出版状态已出版 - 11月 2026
已对外发布

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