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Reprogramming systemic and local immune function to empower immunotherapy against glioblastoma.

Songlei ZhouYukun HuangYu ChenYipu LiuLaozhi XieYang YouShiqiang TongJianpei XuGan JiangQingxiang SongNi MeiFenfen MaXiao-Ling GaoHong-Zhuan ChenJun Chen
Published in: Nature communications (2023)
The limited benefits of immunotherapy against glioblastoma (GBM) is closely related to the paucity of T cells in brain tumor bed. Both systemic and local immunosuppression contribute to the deficiency of tumor-infiltrating T cells. However, the current studies focus heavily on the local immunosuppressive tumor microenvironment but not on the co-existence of systemic immunosuppression. Here, we develop a nanostructure named Nano-reshaper to co-encapsulate lymphopenia alleviating agent cannabidiol and lymphocyte recruiting cytokine LIGHT. The results show that Nano-reshaper increases the number of systemic T cells and improves local T-cell recruitment condition, thus greatly increasing T-cell infiltration. When combined with immune checkpoint inhibitor, this therapeutic modality achieves 83.3% long-term survivors without recurrence in GBM models in male mice. Collectively, this work unveils that simultaneous reprogramming of systemic and local immune function is critical for T-cell based immunotherapy and provides a clinically translatable option for combating brain tumors.
Keyphrases
  • young adults
  • drug induced
  • peripheral blood
  • free survival