Degrade to Display: Coupling Checkpoint Degradation with Exogenous Antigen Presentation to Boost Antitumor Immunity.
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CAR-T cell therapy research
Nanoplatforms for cancer theranostics
Cancer Immunotherapy and Biomarkers
Membrane and extracellular targeted protein degradation (meTPD) has emerged as a revolutionary therapeutic modality against cancer, enabling the lysosomal clearance of traditionally undruggable oncoge
APA
Yicong Ma, Jianfei Jiang, Yu Han (2026). Degrade to Display: Coupling Checkpoint Degradation with Exogenous Antigen Presentation to Boost Antitumor Immunity.. ACS chemical biology. https://doi.org/10.1021/acschembio.6c00191
MLA
Yicong Ma, et al.. "Degrade to Display: Coupling Checkpoint Degradation with Exogenous Antigen Presentation to Boost Antitumor Immunity.." ACS chemical biology, 2026.
PMID
42023934 ↗
Abstract 한글 요약
Membrane and extracellular targeted protein degradation (meTPD) has emerged as a revolutionary therapeutic modality against cancer, enabling the lysosomal clearance of traditionally undruggable oncogenic targets. However, the therapeutic potential of the current meTPD method is frequently compromised by its reliance on loss-of-function elimination in the face of tumor immunosuppression and low immunogenicity. This In Focus article highlights the development of the intratumoral vaccination chimera (iVAC), a "meTPD-Plus" platform that advances beyond target elimination to actively reprogram tumor immunogenicity. By coupling the degradation of PD-L1 with the cross-presentation of exogenous antigens within tumors, iVAC chemically reprograms cancer cells into pseudo antigen-presenting cell entities (pseudo-APCs) capable of engaging bystander memory T cells. This dual-mechanism approach simultaneously relieves checkpoint-mediated immune suppression and enhances tumor antigen presentation, thereby redirecting viral-specific bystander T cells toward tumor recognition and establishing durable, systemic antitumor immunity.
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