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BAG6 restricts pancreatic cancer progression by suppressing the release of IL33-presenting extracellular vesicles and the activation of mast cells.
Alashkar Alhamwe, Bilal; Ponath, Viviane; Alhamdan, Fahd; Dörsam, Bastian; Landwehr, Clara; Linder, Manuel; Pauck, Kim; Miethe, Sarah; Garn, Holger; Finkernagel, Florian; Brichkina, Anna; Lauth, Matthias; Tiwari, Dinesh Kumar; Buchholz, Malte; Bachurski, Daniel; Elmshäuser, Sabrina; Nist, Andrea; Stiewe, Thorsten; Pogge von Strandmann, Lisa; Szymanski, Witold; Beutgen, Vanessa; Graumann, Johannes; Teply-Szymanski, Julia; Keber, Corinna; Denkert, Carsten; Jacob, Ralf; Preußer, Christian; Pogge von Strandmann, Elke.
Afiliação
  • Alashkar Alhamwe B; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Ponath V; Core Facility Extracellular Vesicles, Philipps-University, 35043, Marburg, Germany.
  • Alhamdan F; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Dörsam B; Core Facility Extracellular Vesicles, Philipps-University, 35043, Marburg, Germany.
  • Landwehr C; Department of Anesthesiology, Critical Care, and Pain Medicine, Cardiac Anesthesia Division, Boston Children's Hospital, Boston, USA.
  • Linder M; Department of Immunology and Anaesthesia, Harvard Medical School, Boston, MA, USA.
  • Pauck K; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Miethe S; Core Facility Extracellular Vesicles, Philipps-University, 35043, Marburg, Germany.
  • Garn H; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Finkernagel F; Core Facility Extracellular Vesicles, Philipps-University, 35043, Marburg, Germany.
  • Brichkina A; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Lauth M; Core Facility Extracellular Vesicles, Philipps-University, 35043, Marburg, Germany.
  • Tiwari DK; Translational Inflammation Research Division & Core Facility for Single Cell Multiomics, Philipps-University, 35043, Marburg, Germany.
  • Buchholz M; Translational Inflammation Research Division & Core Facility for Single Cell Multiomics, Philipps-University, 35043, Marburg, Germany.
  • Bachurski D; Translational Inflammation Research Division & Core Facility for Single Cell Multiomics, Philipps-University, 35043, Marburg, Germany.
  • Elmshäuser S; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
  • Nist A; Core Facility Bioinformatics, Philipps-University, 35043, Marburg, Germany.
  • Stiewe T; Clinic for Gastroenterology, Endocrinology and Metabolism; Center for Tumor and Immune Biology, Philipps-University, 35043, Marburg, Germany.
  • Pogge von Strandmann L; Institute of Systems Immunology, Philipps-University, 35043, Marburg, Germany.
  • Szymanski W; Clinic for Gastroenterology, Endocrinology and Metabolism; Center for Tumor and Immune Biology, Philipps-University, 35043, Marburg, Germany.
  • Beutgen V; Clinic for Gastroenterology, Endocrinology and Metabolism; Center for Tumor and Immune Biology, Philipps-University, 35043, Marburg, Germany.
  • Graumann J; Clinic for Gastroenterology, Endocrinology and Metabolism; Center for Tumor and Immune Biology, Philipps-University, 35043, Marburg, Germany.
  • Teply-Szymanski J; Cluster of Excellence on Cellular Stress Responses in Aging-Associated Diseases (CECAD), University of Cologne, Cologne, Germany.
  • Keber C; Institute of Molecular Oncology and Genomics Core Facility, Member of the German Center for Lung Research (DZL), Philipps-University, 35043, Marburg, Germany.
  • Denkert C; Institute of Molecular Oncology and Genomics Core Facility, Member of the German Center for Lung Research (DZL), Philipps-University, 35043, Marburg, Germany.
  • Jacob R; Institute of Molecular Oncology and Genomics Core Facility, Member of the German Center for Lung Research (DZL), Philipps-University, 35043, Marburg, Germany.
  • Preußer C; Institute of Lung Health, Justus Liebig University, 35392, Giessen, Germany.
  • Pogge von Strandmann E; Institute for Tumor Immunology, Philipps-University, 35043, Marburg, Germany.
Cell Mol Immunol ; 2024 Jun 28.
Article em En | MEDLINE | ID: mdl-38942797
ABSTRACT
Recent studies reveal a critical role of tumor cell-released extracellular vesicles (EVs) in pancreatic cancer (PC) progression. However, driver genes that direct EV function, the EV-recipient cells, and their cellular response to EV uptake remain to be identified. Therefore, we studied the role of Bcl-2-associated-anthanogene 6 (BAG6), a regulator of EV biogenesis for cancer progression. We used a Cre recombinase/LoxP-based reporter system in combination with single-cell RNA sequencing to monitor in vivo EV uptake and tumor microenvironment (TME) changes in mouse models for pancreatic ductal adenocarcinoma (PDAC) in a Bag6 pro- or deficient background. In vivo data were validated using mouse and human organoids and patient samples. Our data demonstrated that Bag6-deficient subcutaneous and orthotopic PDAC tumors accelerated tumor growth dependent on EV release. Mechanistically, this was attributed to mast cell (MC) activation via EV-associated IL33. Activated MCs promoted tumor cell proliferation and altered the composition of the TME affecting fibroblast polarization and immune cell infiltration. Tumor cell proliferation and fibroblast polarization were mediated via the MC secretome containing high levels of PDGF and CD73. Patients with high BAG6 gene expression and high protein plasma level have a longer overall survival indicating clinical relevance. The current study revealed a so far unknown tumor-suppressing activity of BAG6 in PDAC. Bag6-deficiency allowed the release of EV-associated IL33 which modulate the TME via MC activation promoting aggressive tumor growth. MC depletion using imatinib diminished tumor growth providing a scientific rationale to consider imatinib for patients stratified with low BAG6 expression and high MC infiltration. EVs derived from BAG6-deficient pancreatic cancer cells induce MC activation via IL33/Il1rl1. The secretome of activated MCs induces tumor proliferation and changes in the TME, particularly shifting fibroblasts into an inflammatory cancer-associated fibroblast (iCAF) phenotype. Blocking EVs or depleting MCs restricts tumor growth.
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Texto completo: 1 Bases de dados: MEDLINE Idioma: En Revista: Cell Mol Immunol Assunto da revista: ALERGIA E IMUNOLOGIA Ano de publicação: 2024 Tipo de documento: Article País de afiliação: Alemanha
Texto completo
Adicionar na Minha BVS
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Bases de dados: MEDLINE Idioma: En Revista: Cell Mol Immunol Assunto da revista: ALERGIA E IMUNOLOGIA Ano de publicação: 2024 Tipo de documento: Article País de afiliação: Alemanha