Fibrotic enzymes modulate wound-induced skin tumorigenesis

Lisette Van Hove; Kim Lecomte; Jana Roels; Niels Vandamme; Hanna-Kaisa Vikkula; Isabelle Hoorens; Katia Ongenae; Tino Hochepied; Giacomo Donati; Yvan Saeys; Sven R Quist; Fiona M Watt; Geert van Loo; Esther Hoste

doi:10.15252/embr.202051573

Fibrotic enzymes modulate wound-induced skin tumorigenesis

Lisette Van Hove, Kim Lecomte, Jana Roels, Niels Vandamme, Hanna-Kaisa Vikkula, Isabelle Hoorens, Katia Ongenae, Tino Hochepied, Giacomo Donati, Yvan Saeys, Sven R Quist, Fiona M Watt, Geert van Loo, Esther Hoste

Unit for Cellular and Molecular Pathophysiology, VIB Center for Inflammation Research, Ghent, Belgium.
Department of Endocrinology and Internal Medicine, University Hospital Ghent and Faculty of Medicine, Ghent University, Ghent, Belgium.
University of Turin
Biotechnology Research Center, Department of Molecular Medicine, Pasteur Institute of Iran, Tehran, Iran.
ALS Center, Rita Levi Montalcini Department of Neuroscience, University of Turin, Turin, Italy; Azienda Ospedaliero Universitaria Città della Salute e della Scienza di Torino, Turin, Italy; Neuroscience Institute of Turin (NIT), Turin, Italy.
Centre for Stem Cells and Regenerative Medicine
King's College London
Epithelial Cell Biology Laboratory, Cancer Research UK Cambridge Research Institute, Li Ka Shing Centre, Robinson Way, Cambridge CB2 0RE, UK; Clinic of Dermatology and Venereology, Otto-von-Guericke University, Magdeburg, Leipziger Strasse 44, 39120 Magdeburg, Germany.
Ghent Institute for Functional and Metabolic Imaging (GIfMI), Ghent University, Ghent, Belgium.
Department of Biomedical Molecular Biology

Research output: Contribution to journal › Article › peer-review

12 Citations (Scopus)

Abstract

Fibroblasts are a major component of the microenvironment of most solid tumours. Recent research elucidated a large heterogeneity and plasticity of activated fibroblasts, indicating that their role in cancer initiation, growth and metastasis is complex and context-dependent. Here, we performed genome-wide expression analysis comparing fibroblasts in normal, inflammatory and tumour-associated skin. Cancer-associated fibroblasts (CAFs) exhibit a fibrotic gene signature in wound-induced tumours, demonstrating persistent extracellular matrix (ECM) remodelling within these tumours. A top upregulated gene in mouse CAFs encodes for PRSS35, a protease capable of collagen remodelling. In human skin, we observed PRSS35 expression uniquely in the stroma of high-grade squamous cell carcinomas. Ablation of PRSS35 in mouse models of wound- or chemically-induced tumorigenesis resulted in aberrant collagen composition in the ECM and increased tumour incidence. Our results indicate that fibrotic enzymes expressed by CAFs can regulate squamous tumour initiation by remodelling the ECM.

Original language	English
Article number	e51573
Pages (from-to)	e51573
Journal	EMBO Reports
Volume	22
Issue number	5
Early online date	29 Mar 2021
DOIs	https://doi.org/10.15252/embr.202051573
Publication status	Published - 5 May 2021

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title = "Fibrotic enzymes modulate wound-induced skin tumorigenesis",

abstract = "Fibroblasts are a major component of the microenvironment of most solid tumours. Recent research elucidated a large heterogeneity and plasticity of activated fibroblasts, indicating that their role in cancer initiation, growth and metastasis is complex and context-dependent. Here, we performed genome-wide expression analysis comparing fibroblasts in normal, inflammatory and tumour-associated skin. Cancer-associated fibroblasts (CAFs) exhibit a fibrotic gene signature in wound-induced tumours, demonstrating persistent extracellular matrix (ECM) remodelling within these tumours. A top upregulated gene in mouse CAFs encodes for PRSS35, a protease capable of collagen remodelling. In human skin, we observed PRSS35 expression uniquely in the stroma of high-grade squamous cell carcinomas. Ablation of PRSS35 in mouse models of wound- or chemically-induced tumorigenesis resulted in aberrant collagen composition in the ECM and increased tumour incidence. Our results indicate that fibrotic enzymes expressed by CAFs can regulate squamous tumour initiation by remodelling the ECM.",

author = "{Van Hove}, Lisette and Kim Lecomte and Jana Roels and Niels Vandamme and Hanna-Kaisa Vikkula and Isabelle Hoorens and Katia Ongenae and Tino Hochepied and Giacomo Donati and Yvan Saeys and Quist, {Sven R} and Watt, {Fiona M} and {van Loo}, Geert and Esther Hoste",

note = "Funding Information: We thank Laetitia Bellen, Dimitri Huygebaert and Dieter Vanhede for animal care, and all members of the van Loo laboratory for suggestions and discussions. We acknowledge the VIB Bioimaging core for their help with imaging and analysis. L.v.H is supported by an FWO FR fellowship, I.H. is supported by an FWO postdoctoral fellowship. G.D. is supported by AIRC MFAG 2018. E.H. is supported by an FWO postdoctoral fellowship and a CRIG Young‐Investigator grant. Research in the van Loo lab is financed by research grants from the FWO, Stichting tegen Kanker, Kom op Tegen Kanker and the “Concerted Research Actions” (GOA) of the Ghent University. Publisher Copyright: {\textcopyright} 2021 The Authors Copyright: Copyright 2021 Elsevier B.V., All rights reserved.",

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doi = "10.15252/embr.202051573",

language = "English",

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T1 - Fibrotic enzymes modulate wound-induced skin tumorigenesis

AU - Van Hove, Lisette

AU - Lecomte, Kim

AU - Roels, Jana

AU - Vandamme, Niels

AU - Vikkula, Hanna-Kaisa

AU - Hoorens, Isabelle

AU - Ongenae, Katia

AU - Hochepied, Tino

AU - Donati, Giacomo

AU - Saeys, Yvan

AU - Quist, Sven R

AU - Watt, Fiona M

AU - van Loo, Geert

AU - Hoste, Esther

N1 - Funding Information: We thank Laetitia Bellen, Dimitri Huygebaert and Dieter Vanhede for animal care, and all members of the van Loo laboratory for suggestions and discussions. We acknowledge the VIB Bioimaging core for their help with imaging and analysis. L.v.H is supported by an FWO FR fellowship, I.H. is supported by an FWO postdoctoral fellowship. G.D. is supported by AIRC MFAG 2018. E.H. is supported by an FWO postdoctoral fellowship and a CRIG Young‐Investigator grant. Research in the van Loo lab is financed by research grants from the FWO, Stichting tegen Kanker, Kom op Tegen Kanker and the “Concerted Research Actions” (GOA) of the Ghent University. Publisher Copyright: © 2021 The Authors Copyright: Copyright 2021 Elsevier B.V., All rights reserved.

PY - 2021/5/5

Y1 - 2021/5/5

N2 - Fibroblasts are a major component of the microenvironment of most solid tumours. Recent research elucidated a large heterogeneity and plasticity of activated fibroblasts, indicating that their role in cancer initiation, growth and metastasis is complex and context-dependent. Here, we performed genome-wide expression analysis comparing fibroblasts in normal, inflammatory and tumour-associated skin. Cancer-associated fibroblasts (CAFs) exhibit a fibrotic gene signature in wound-induced tumours, demonstrating persistent extracellular matrix (ECM) remodelling within these tumours. A top upregulated gene in mouse CAFs encodes for PRSS35, a protease capable of collagen remodelling. In human skin, we observed PRSS35 expression uniquely in the stroma of high-grade squamous cell carcinomas. Ablation of PRSS35 in mouse models of wound- or chemically-induced tumorigenesis resulted in aberrant collagen composition in the ECM and increased tumour incidence. Our results indicate that fibrotic enzymes expressed by CAFs can regulate squamous tumour initiation by remodelling the ECM.

AB - Fibroblasts are a major component of the microenvironment of most solid tumours. Recent research elucidated a large heterogeneity and plasticity of activated fibroblasts, indicating that their role in cancer initiation, growth and metastasis is complex and context-dependent. Here, we performed genome-wide expression analysis comparing fibroblasts in normal, inflammatory and tumour-associated skin. Cancer-associated fibroblasts (CAFs) exhibit a fibrotic gene signature in wound-induced tumours, demonstrating persistent extracellular matrix (ECM) remodelling within these tumours. A top upregulated gene in mouse CAFs encodes for PRSS35, a protease capable of collagen remodelling. In human skin, we observed PRSS35 expression uniquely in the stroma of high-grade squamous cell carcinomas. Ablation of PRSS35 in mouse models of wound- or chemically-induced tumorigenesis resulted in aberrant collagen composition in the ECM and increased tumour incidence. Our results indicate that fibrotic enzymes expressed by CAFs can regulate squamous tumour initiation by remodelling the ECM.

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DO - 10.15252/embr.202051573

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SP - e51573

JO - EMBO Reports

JF - EMBO Reports

IS - 5

M1 - e51573

ER -

Fibrotic enzymes modulate wound-induced skin tumorigenesis

Abstract

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