Nature Communications (Nov 2024)

In situ editing of tumour cell membranes induces aggregation and capture of PD-L1 membrane proteins for enhanced cancer immunotherapy

  • Chunping Mao,
  • Fuan Deng,
  • Wanning Zhu,
  • Leiming Xie,
  • Yijun Wang,
  • Guoyin Li,
  • Xingke Huang,
  • Jiahui Wang,
  • Yue Song,
  • Ping Zeng,
  • Zhenpeng He,
  • Jingnan Guo,
  • Yao Suo,
  • Yujing Liu,
  • Zhuo Chen,
  • Mingxi Yao,
  • Lu Zhang,
  • Jun Shen

DOI
https://doi.org/10.1038/s41467-024-54081-9
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 20

Abstract

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Abstract Immune checkpoint blockade (ICB) therapy has emerged as a new therapeutic paradigm for a variety of advanced cancers, but wide clinical application is hindered by low response rate. Here we use a peptide-based, biomimetic, self-assembly strategy to generate a nanoparticle, TPM1, for binding PD-L1 on tumour cell surface. Upon binding with PD-L1, TPM1 transforms into fibrillar networks in situ to facilitate the aggregation of both bound and unbound PD-L1, thereby resulting in the blockade of the PD-1/PD-L1 pathway. Characterizations of TPM1 manifest a prolonged retention in tumour ( > 7 days) and anti-cancer effects associated with reinvigorating CD8+ T cells in multiple mice tumour models. Our results thus hint TPM1 as a potential strategy for enhancing the ICB efficacy.