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Inorganic nanosheets facilitate humoral immunity against medical implant infections by modulating immune co-stimulatory pathways

  • Chuang Yang
  • , Yao Luo
  • , Hao Shen
  • , Min Ge
  • , Jin Tang
  • , Qiaojie Wang
  • , Han Lin*
  • , Jianlin Shi*
  • , Xianlong Zhang*
  • *此作品的通讯作者

科研成果: 期刊稿件文章同行评审

摘要

Strategies to manipulate immune cell co-inhibitory or co-activating signals have revolutionized immunotherapy. However, certain immunologically cold diseases, such as bacterial biofilm infections of medical implants are hard to target due to the complexity of the immune co-stimulatory pathways involved. Here we show that two-dimensional manganese chalcogenophosphates MnPSe3 (MPS) nanosheets modified with polyvinylpyrrolidone (PVP) are capable of triggering a strong anti-bacterial biofilm humoral immunity in a mouse model of surgical implant infection via modulating antigen presentation and costimulatory molecule expression in the infectious microenvironment (IME). Mechanistically, the PVP-modified MPS (MPS-PVP) damages the structure of the biofilm which results in antigen exposure by generating reactive oxidative species, while changing the balance of immune-inhibitory (IL4I1 and CD206) and co-activator signals (CD40, CD80 and CD69). This leads to amplified APC priming and antigen presentation, resulting in biofilm-specific humoral immune and memory responses. In our work, we demonstrate that pre-surgical neoadjuvant immunotherapy utilizing MPS-PVP successfully mitigates residual and recurrent infections following removal of the infected implants. This study thus offers an alternative to replace antibiotics against hard-to-treat biofilm infections.

源语言英语
文章编号4866
期刊Nature Communications
13
1
DOI
出版状态已出版 - 12月 2022
已对外发布

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