Abstract

AbstractWith the development of oncology, immunotherapy holds great promise for tumor treatment. However, immunogenic cell death (ICD), an important stimulator of immune response, often fails to trigger effective immunotherapy. Herein, a strategy to cause endoplasmic reticulum (ER) stress for further amplifying ICD is reported. A porous organic framework‐based nanoplatform (PLGH‐TER) with good targeting ER ability for chemiluminescence resonance energy transfer (CRET) based‐photodynamic therapy (PDT) is developed, which solves the limitations of the restricted penetration of light and suboptimal bioavailability of commonly used photosensitizers (PS). Once accumulated in ER, PLGH‐TER activates the translation from glucose to H2O2 for starvation therapy and further elicit CRET‐based‐PDT, which results in ER stress and amplified ICD ultimately. Then, the amplified ICD promotes the release of damage‐associated molecular patterns , realizing enhanced immunotherapy. Consequently, PLGH‐TER can achieve directional destruction on ER and inhibit tumor invasion and recurrence, which expands the application of porous organic framework for tumor immunotherapy.

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