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Progranulin mediates immune evasion of pancreatic ductal adenocarcinoma through regulation of MHCI expression.


ABSTRACT: Immune evasion is indispensable for cancer initiation and progression, although its underlying mechanisms in pancreatic ductal adenocarcinoma (PDAC) are not fully known. Here, we characterize the function of tumor-derived PGRN in promoting immune evasion in primary PDAC. Tumor- but not macrophage-derived PGRN is associated with poor overall survival in PDAC. Multiplex immunohistochemistry shows low MHC class I (MHCI) expression and lack of CD8+ T cell infiltration in PGRN-high tumors. Inhibition of PGRN abrogates autophagy-dependent MHCI degradation and restores MHCI expression on PDAC cells. Antibody-based blockade of PGRN in a PDAC mouse model remarkably decelerates tumor initiation and progression. Notably, tumors expressing LCMV-gp33 as a model antigen are sensitized to gp33-TCR transgenic T cell-mediated cytotoxicity upon PGRN blockade. Overall, our study shows a crucial function of tumor-derived PGRN in regulating immunogenicity of primary PDAC.

SUBMITTER: Cheung PF 

PROVIDER: S-EPMC8748938 | biostudies-literature | 2022 Jan

REPOSITORIES: biostudies-literature

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Progranulin mediates immune evasion of pancreatic ductal adenocarcinoma through regulation of MHCI expression.

Cheung Phyllis F PF   Yang JiaJin J   Fang Rui R   Borgers Arianna A   Krengel Kirsten K   Stoffel Anne A   Althoff Kristina K   Yip Chi Wai CW   Siu Elaine H L EHL   Ng Linda W C LWC   Lang Karl S KS   Cham Lamin B LB   Engel Daniel R DR   Soun Camille C   Cima Igor I   Scheffler Björn B   Striefler Jana K JK   Sinn Marianne M   Bahra Marcus M   Pelzer Uwe U   Oettle Helmut H   Markus Peter P   Smeets Esther M M EMM   Aarntzen Erik H J G EHJG   Savvatakis Konstantinos K   Liffers Sven-Thorsten ST   Lueong Smiths S SS   Neander Christian C   Bazarna Anna A   Zhang Xin X   Paschen Annette A   Crawford Howard C HC   Chan Anthony W H AWH   Cheung Siu Tim ST   Siveke Jens T JT  

Nature communications 20220110 1


Immune evasion is indispensable for cancer initiation and progression, although its underlying mechanisms in pancreatic ductal adenocarcinoma (PDAC) are not fully known. Here, we characterize the function of tumor-derived PGRN in promoting immune evasion in primary PDAC. Tumor- but not macrophage-derived PGRN is associated with poor overall survival in PDAC. Multiplex immunohistochemistry shows low MHC class I (MHCI) expression and lack of CD8<sup>+</sup> T cell infiltration in PGRN-high tumors.  ...[more]

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