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PD-L1-targeted photodynamic therapy orchestrates checkpoint blockade and immunogenic cell death for synergistic cancer immunotherapy.

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Redox biology 📖 저널 OA 100% 2024: 2/2 OA 2025: 24/24 OA 2026: 32/32 OA 2024~2026 2026 Vol.91() p. 104075 cited 1 OA Nanoplatforms for cancer theranostic
TL;DR This PD-L1-targeted PDTAC achieved immune checkpoint blockade and ICD induction in a single therapeutic mode using one molecular species, presenting a novel strategy for combinational immunotherapy, particularly in immune cold tumors.
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PubMed DOI PMC OpenAlex Semantic 마지막 보강 2026-04-30
OpenAlex 토픽 · Nanoplatforms for cancer theranostics Photodynamic Therapy Research Studies Cancer Immunotherapy and Biomarkers

Liu S, Yang Z, Wang B, Huan S, Li Z, Wei X

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This PD-L1-targeted PDTAC achieved immune checkpoint blockade and ICD induction in a single therapeutic mode using one molecular species, presenting a novel strategy for combinational immunotherapy, p

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APA Sijin Liu, Zhaoting Yang, et al. (2026). PD-L1-targeted photodynamic therapy orchestrates checkpoint blockade and immunogenic cell death for synergistic cancer immunotherapy.. Redox biology, 91, 104075. https://doi.org/10.1016/j.redox.2026.104075
MLA Sijin Liu, et al.. "PD-L1-targeted photodynamic therapy orchestrates checkpoint blockade and immunogenic cell death for synergistic cancer immunotherapy.." Redox biology, vol. 91, 2026, pp. 104075.
PMID 41666678 ↗

Abstract

Inhibiting the PD1/PD-L1 interaction is crucial for developing novel cancer immunotherapies, particularly to reduce systemic toxicity and enhance patient response rates. In this study, we designed and synthesized Photodegradation-Targeting Chimeras (PDTACs) by conjugating a clinically approved photosensitizer, verteporfin, to a PD-L1-targeted peptide. Our optimized chimera, PPA-VPF, demonstrates a dual mechanism of action in cancer immunotherapy, resulting from singlet oxygen generated under light irradiation. The proximity-generated singlet oxygen effectively degrades PD-L1 in cancer cells through immediate protein breakdown and resulted in subsequent lysosomal-dependent degradation hours after irradiation. Additionally, the non-proximity-generated singlet oxygen induces immunogenic cell death (ICD) through cytotoxic effects. In mouse models with immune cold tumors, PPA-VPF elicited robust adaptive antitumor immunity and effectively inhibited the growth of both primary and distant tumors. This PD-L1-targeted PDTAC achieved immune checkpoint blockade and ICD induction in a single therapeutic mode using one molecular species, presenting a novel strategy for combinational immunotherapy, particularly in immune cold tumors.

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