Author
Listed:
- Rongrong Zhao
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Ying Hou
(University of Jinan)
- Boyan Li
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Ziwen Pan
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Jiawei Qiu
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Qingtong Wang
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Yanhua Qi
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Zhe Han
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Hongyu Zhao
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Hong Liu
(University of Jinan
Shandong University)
- Weijia Zhou
(University of Jinan)
- Gang Li
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
- Hao Xue
(Shandong University
Shandong Key Laboratory of Brain Health and Function Remodelling)
Abstract
Glioblastoma (GBM) poses significant therapeutic challenges due to its hypoxic and immunosuppressive tumour microenvironment (TME), low immunogenicity and physical barriers. While combining photodynamic therapy (PDT) with immunotherapy holds promise, its efficacy is hampered by insufficient immune activation. In this study, we develop a multifunctional photodynamic-enhanced biomimetic intelligent nanoplatform (FBFO@HM@aOPN) responsive to the TME. The nanoplatform consists of a dual-enzyme nanozyme encapsulated in a prokaryotic-eukaryotic hybrid membrane, further modified with a pH-sensitive tumor-targeting antibody. After systemic administration, FBFO@HM@aOPN selectively accumulates in the GBM through vascular regulation and extracellular matrix (ECM) remodelling while generating oxygen to alleviate hypoxia. Crucially, the platform concurrently induces immunogenic death in tumour cells and reprograms protumoral macrophages to antitumor phenotypes. This dual action robustly activates both innate and adaptive immunity, significantly inhibiting GBM growth. Furthermore, when combined with anti-PD1 immunotherapy, the nanoplatform dramatically boosts the treatment effect and effectively prevents postsurgical tumour recurrence. Therefore, our work offers a multimodal platform for stimulating anti-tumour immunity, with potential applicability for GBM patients.
Suggested Citation
Rongrong Zhao & Ying Hou & Boyan Li & Ziwen Pan & Jiawei Qiu & Qingtong Wang & Yanhua Qi & Zhe Han & Hongyu Zhao & Hong Liu & Weijia Zhou & Gang Li & Hao Xue, 2025.
"Bioengineered hybrid dual-targeting nanoparticles reprogram the tumour microenvironment for deep glioblastoma photodynamic therapy,"
Nature Communications, Nature, vol. 16(1), pages 1-22, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-63081-2
DOI: 10.1038/s41467-025-63081-2
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