JUN mediates the senescence associated secretory phenotype and immune cell recruitment to prevent prostate cancer progression

Torben Redmer; Martin Raigel; Christina Sternberg; Roman Ziegler; Clara Probst; Desiree Lindner; Astrid Aufinger; Tanja Limberger; Karolina Trachtova; Petra Kodajova; Sandra Högler; Michaela Schlederer; Stefan Stoiber; Monika Oberhuber; Marco Bolis; Heidi A. Neubauer; Sara Miranda; Martina Tomberger; Nora S. Harbusch; Ines Garces de Los Fayos Alonso; Richard Moriggl; Jean-Philippe Theurillat; Boris Tichy; Vojtech Bystry; Jenny L Persson; Stephan Mathas; Fritz Aberger; Birgit Strobl; Sarka Pospisilova; Olaf Merkel; Gerda Egger; Sabine Lagger; Lukas Kenner

doi:10.1186/s12943-024-02022-x

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Title (en)

JUN mediates the senescence associated secretory phenotype and immune cell recruitment to prevent prostate cancer progression

Language

English

Description (en)

Prostate cancer develops through malignant transformation of the prostate epithelium in a stepwise, mutation-driven process. Although activator protein-1 transcription factors such as JUN have been implicated as potential oncogenic drivers, the molecular programs contributing to prostate cancer progression are not fully understood.We analyzed JUN expression in clinical prostate cancer samples across different stages and investigated its functional role in a Pten-deficient mouse model. We performed histopathological examinations, transcriptomic analyses and explored the senescence-associated secretory phenotype in the tumor microenvironment.Elevated JUN levels characterized early-stage prostate cancer and predicted improved survival in human and murine samples. Immune-phenotyping of Pten-deficient prostates revealed high accumulation of tumor-infiltrating leukocytes, particularly innate immune cells, neutrophils and macrophages as well as high levels of STAT3 activation and IL-1? production. Jun depletion in a Pten-deficient background prevented immune cell attraction which was accompanied by significant reduction of active STAT3 and IL-1? and accelerated prostate tumor growth. Comparative transcriptome profiling of prostate epithelial cells revealed a senescence-associated gene signature, upregulation of pro-inflammatory processes involved in immune cell attraction and of chemokines such as IL-1?, TNF-?, CCL3 and CCL8 in Pten-deficient prostates. Strikingly, JUN depletion reversed both the senescence-associated secretory phenotype and senescence-associated immune cell infiltration but had no impact on cell cycle arrest. As a result, JUN depletion in Pten-deficient prostates interfered with the senescence-associated immune clearance and accelerated tumor growth.Our results suggest that JUN acts as tumor-suppressor and decelerates the progression of prostate cancer by transcriptional regulation of senescence- and inflammation-associated genes. This study opens avenues for novel treatment strategies that could impede disease progression and improve patient outcomes.

Keywords (en)

Male; Prostatic Neoplasmspathologygeneticsmetabolism; Animals; Mice; Humans; PTEN Phosphohydrolasegeneticsmetabolism; Disease Progression; Tumor Microenvironmentimmunology; Senescence-Associated Secretory Phenotype; Proto-Oncogene Proteins c-junmetabolism; Gene Expression Regulation, Neoplastic; Cell Line, Tumor; Gene Expression Profiling; Cellular Senescencegenetics; Disease Models, Animal

DOI

10.1186/s12943-024-02022-x

Author of the digital object

Torben Redmer (University of Veterinary Medicine Vienna)

Lukas Kenner (University of Veterinary Medicine Vienna / Medical University of Vienna / CBmed GmbH)

Sabine Lagger (University of Veterinary Medicine Vienna)

Gerda Egger (Medical University of Vienna)

Olaf Merkel (Medical University of Vienna)

Sarka Pospisilova (Masaryk University)

Birgit Strobl (University of Veterinary Medicine Vienna)

Fritz Aberger (Paris-Lodron University of Salzburg)

Stephan Mathas

Jenny L Persson (Umeå University / Malmö Universitet)

Vojtech Bystry (Masaryk University)

Boris Tichy (Masaryk University)

Jean-Philippe Theurillat

Richard Moriggl (Paris-Lodron University of Salzburg)

Ines Garces de Los Fayos Alonso (University of Veterinary Medicine Vienna / Medical University of Vienna)

Nora S. Harbusch (CBmed GmbH)

Martina Tomberger (CBmed GmbH)

Sara Miranda (University of Veterinary Medicine Vienna)

Heidi A. Neubauer (University of Veterinary Medicine Vienna)

Marco Bolis

Monika Oberhuber (CBmed GmbH)

Stefan Stoiber (Medical University Vienna)

Michaela Schlederer (Medical University of Vienna)

Sandra Högler (University of Veterinary Medicine Vienna)

Petra Kodajova (University of Veterinary Medicine Vienna)

Karolina Trachtova (Medical University of Vienna / Masaryk University)

Tanja Limberger (Medical University of Vienna)

Astrid Aufinger (Medical University Vienna)

Desiree Lindner (University of Veterinary Medicine Vienna / Medical University of Vienna)

Clara Probst (University of Veterinary Medicine Vienna / Medical University of Vienna)

Roman Ziegler (University of Veterinary Medicine Vienna / Charles University)

Martin Raigel (University of Veterinary Medicine Vienna / Medical University of Vienna)

Christina Sternberg (University of Veterinary Medicine Vienna / Medical University of Vienna / University of Kiel)

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4.0 MB

Licence Selected

CC BY 4.0 International

Type of publication

Article

Name of Publication (en)

Molecular Cancer

Pages or Volume

21

Volume

23

Number

1

Publisher

BMC

Publication Date

2024

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Persistent identifier
https://phaidra.vetmeduni.ac.at/o:3187
DOI
https://doi.org/10.1186/s12943-024-02022-x
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Vetmeduni Vienna Universitätsbibliothek

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04.07.2024 09:20:13 UTC
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