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Hyperglycosylation of prosaposin in tumor dendritic cells drives immune escape

Pankaj Sharma, Xiaolong Zhang, Kévin Ly, Ji Hyung Kim, Qi Wan, Jessica Kim, Mumeng Lou, Lisa Kain, Luc Teyton, Florian Winau

2024Science68 citationsDOIOpen Access PDF

Abstract

Tumors develop strategies to evade immunity by suppressing antigen presentation. In this work, we show that prosaposin (pSAP) drives CD8 T cell-mediated tumor immunity and that its hyperglycosylation in tumor dendritic cells (DCs) leads to cancer immune escape. We found that lysosomal pSAP and its single-saposin cognates mediated disintegration of tumor cell-derived apoptotic bodies to facilitate presentation of membrane-associated antigen and T cell activation. In the tumor microenvironment, transforming growth factor-β (TGF-β) induced hyperglycosylation of pSAP and its subsequent secretion, which ultimately caused depletion of lysosomal saposins. pSAP hyperglycosylation was also observed in tumor-associated DCs from melanoma patients, and reconstitution with pSAP rescued activation of tumor-infiltrating T cells. Targeting DCs with recombinant pSAP triggered tumor protection and enhanced immune checkpoint therapy. Our studies demonstrate a critical function of pSAP in tumor immunity and may support its role in immunotherapy.

Topics & Concepts

Immune systemTumor microenvironmentCancer immunotherapyImmunotherapyAntigen presentationSecretionTumor antigenDendritic cellImmunityAntigenBiologyCD8Cytotoxic T cellCell biologyT cellAcquired immune systemCancer researchImmunologyIn vitroBiochemistryImmunotherapy and Immune ResponsesT-cell and B-cell ImmunologyImmune Cell Function and Interaction
Hyperglycosylation of prosaposin in tumor dendritic cells drives immune escape | Litcius