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Tumor extracellular vesicles mediate anti-PD-L1 therapy resistance by decoying anti-PD-L1

Jiming Chen, Jie Yang, Wenhui Wang, Danfeng Guo, Chengyan Zhang, Shibo Wang, Xinliang Lu, Xiaofang Huang, Pingli Wang, Gensheng Zhang, Jing Zhang, Jianli Wang, Zhijian Cai

2022Cellular and Molecular Immunology73 citationsDOIOpen Access PDF

Abstract

Abstract PD-L1 + tumor-derived extracellular vesicles (TEVs) cause systemic immunosuppression and possibly resistance to anti-PD-L1 antibody (αPD-L1) blockade. However, whether and how PD-L1 + TEVs mediate αPD-L1 therapy resistance is unknown. Here, we show that PD-L1 + TEVs substantially decoy αPD-L1 and that TEV-bound αPD-L1 is more rapidly cleared by macrophages, causing insufficient blockade of tumor PD-L1 and subsequent αPD-L1 therapy resistance. Inhibition of endogenous production of TEVs by Rab27a or Coro1a knockout reverses αPD-L1 therapy resistance. Either an increased αPD-L1 dose or macrophage depletion mediated by the clinical drug pexidartinib abolishes αPD-L1 therapy resistance. Moreover, in the treatment cycle with the same total treatment dose of αPD-L1, high-dose and low-frequency treatment had better antitumor effects than low-dose and high-frequency treatment, induced stronger antitumor immune memory, and eliminated αPD-L1 therapy resistance. Notably, in humanized immune system mice with human xenograft tumors, both increased αPD-L1 dose and high-dose and low-frequency treatment enhanced the antitumor effects of αPD-L1. Furthermore, increased doses of αPD-L1 and αPD-1 had comparable antitumor effects, but αPD-L1 amplified fewer PD-1 + Treg cells, which are responsible for tumor hyperprogression. Altogether, our results reveal a TEV-mediated mechanism of αPD-L1-specific therapy resistance, thus providing promising strategies to improve αPD-L1 efficacy.

Topics & Concepts

PD-L1BlockadeCancer researchImmune systemCombination therapyPharmacologyMedicineDrug resistanceImmunotherapyImmunologyChemistryBiologyReceptorInternal medicineMicrobiologyExtracellular vesicles in diseaseCancer Immunotherapy and BiomarkersImmunotherapy and Immune Responses
Tumor extracellular vesicles mediate anti-PD-L1 therapy resistance by decoying anti-PD-L1 | Litcius