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Multifunctional copper-light synergistic prodrug nanosystems for specific reprogramming of tumour immunogenic endoplasmic reticulum stress.

Biomaterials 2026 Vol.325() p. 123625

Lu H, Chen W, Jia C, Hu A, Aji A, Wang J, Chen Q, Liang B, Zhou X, Cui W, Jiang L, Dong J

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Inducing lethal endoplasmic reticulum (ER) stress is a key initiative to counteract tumour resistance and induce anti-tumour immunity.

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APA Lu H, Chen W, et al. (2026). Multifunctional copper-light synergistic prodrug nanosystems for specific reprogramming of tumour immunogenic endoplasmic reticulum stress.. Biomaterials, 325, 123625. https://doi.org/10.1016/j.biomaterials.2025.123625
MLA Lu H, et al.. "Multifunctional copper-light synergistic prodrug nanosystems for specific reprogramming of tumour immunogenic endoplasmic reticulum stress.." Biomaterials, vol. 325, 2026, pp. 123625.
PMID 40819601

Abstract

Inducing lethal endoplasmic reticulum (ER) stress is a key initiative to counteract tumour resistance and induce anti-tumour immunity. However, conventional ER stress inducers are largely limited by hypoxia and off-target effects to induce tumour-lethal ER stress. Here, we encapsulated Cu-bridged eosin Y (CuBY) in ER-targeting peptide (pardaxin)-modified mesoporous silica and successfully constructed an oxygen-independent multifunctional copper-light synergistic prodrug nanosystems (MP@CuBY). MP@CuBY is activated to the "on" state within the glutathione-overexpressing tumour microenvironment, causing copper and BY release. Interestingly, released copper can drive oxygen-independent cascade reactions in situ in the ER, resulting in the production of highly toxic O-• and •OH. The BY released can produce O in situ in the ER under laser irradiation. Therefore, type I and type II reactive oxygen species (ROS) generated by MP@CuBY in situ in the ER specifically reprogramed tumour immunogenic ER stress, which significantly activated systemic anti-tumour immunity and long-term immune memory, as well as ensured satisfactory efficacy in synergistically eradicating spinal metastases in conjunction with α-PD-L1 antibody. In conclusion, the well-designed MP@CuBY may represent an advanced design for anti-tumour prodrug nanosystems, providing a novel copper-light synergistic strategy for the specific activation of lethal tumour ER stress.

MeSH Terms

Prodrugs; Endoplasmic Reticulum Stress; Copper; Animals; Humans; Cell Line, Tumor; Light; Mice; Reactive Oxygen Species; Female; Tumor Microenvironment; Neoplasms

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