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Cancer cells under immune attack acquire CD47-mediated adaptive immune resistance independent of the myeloid CD47-SIRPα axis

Oncoimmunology. 2021-11; 
Mark A J M Hendriks, Isabel Britsch, Xiurong Ke, Anne P van Wijngarden, Douwe F Samplonius, Emily M Ploeg, Wijnand Helfrich
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Gene Synthesis … , Inhibrix) were generated by commercial gene synthesis service (GenScript). Fluorescently labeled secondary antibody goat anti-human Ig … In short, DNA fragments encoding scFv MABL and scFv 425 were generated by commercial gene synthesis service (GenScript) based on … Get A Quote

摘要

Cancer cells exploit CD47 overexpression to inhibit phagocytic elimination and neoantigen processing via the myeloid CD47-SIRPα axis and thereby indirectly evade adaptive T cell immunity. Here, we report on a hitherto unrecognized direct immunoinhibitory feature of cancer cell-expressed CD47. We uncovered that in response to IFNγ released during cognate T cell immune attack, cancer cells dynamically enhance CD47 cell surface expression, which coincides with acquiring adaptive immune resistance toward pro-apoptotic effector T cell mechanisms. Indeed, CRISPR/Cas9-mediated CD47-knockout rendered cancer cells more sensitive to cognate T cell immune attack. Subsequently, we developed a cancer-directed strategy to ... More

关键词

CD47, T cell-induced cytotoxicity, bispecific antibody, cancer immunotherapy, resistance