A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea

Planarians have been long known for their regenerative ability, which hinges on pluripotency. Recently, however, the planarian model has been successfully established for routine toxicological screens aimed to assess overproliferation, mutagenicity and tumorigenesis. In this study, we focused on pla...

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Main Authors: Andromeda Van Roten, Amal Zohir Abo-Zeid Barakat, Annelies Wouters, Thao Anh Tran, Stijn Mouton, Jean-Paul Noben, Luca Gentile, Karen Smeets
Format: Article
Language:English
Published: The Company of Biologists 2018-09-01
Series:Disease Models & Mechanisms
Subjects:
Online Access:http://dmm.biologists.org/content/11/9/dmm032573
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spelling doaj-5db661c74ca84511a02fc0d13568462c2020-11-25T02:00:14ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112018-09-0111910.1242/dmm.032573032573A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterraneaAndromeda Van Roten0Amal Zohir Abo-Zeid Barakat1Annelies Wouters2Thao Anh Tran3Stijn Mouton4Jean-Paul Noben5Luca Gentile6Karen Smeets7 Zoology: Biodiversity and Toxicology, Hasselt University–Campus Diepenbeek, Agoralaan 1, Gebouw D, 3590, Diepenbeek, Belgium Planarian Stem Cell Laboratory, Max Planck Institute for Molecular Biomedicine, von Esmarch-str. 54, 48149, Münster, Germany Zoology: Biodiversity and Toxicology, Hasselt University–Campus Diepenbeek, Agoralaan 1, Gebouw D, 3590 Diepenbeek, Belgium Pluripotency and Regeneration Group, Fraunhofer Institute for Biomedical Engineering, Joseph-von-Fraunhofer-Weg 1, 66280, Sulzbach, Germany European Research Institute for the Biology of Ageing, University Medical Center Groningen, University of Groningen, 9713, Groningen, The Netherlands Biomedical Research Institute, Hasselt University and Transnationale Universiteit Limburg, School of Life Sciences, 3590, Diepenbeek, Belgium Planarian Stem Cell Laboratory, Max Planck Institute for Molecular Biomedicine, von Esmarch-str. 54, 48149, Münster, Germany Zoology: Biodiversity and Toxicology, Hasselt University–Campus Diepenbeek, Agoralaan 1, Gebouw D, 3590, Diepenbeek, Belgium Planarians have been long known for their regenerative ability, which hinges on pluripotency. Recently, however, the planarian model has been successfully established for routine toxicological screens aimed to assess overproliferation, mutagenicity and tumorigenesis. In this study, we focused on planarian tumor suppressor genes (TSGs) and their role during chemically induced carcinogenic stress in Schmidtea mediterranea. Combining in silico and proteomic screens with exposure to human carcinogen type 1A agent cadmium (Cd), we showed that many TSGs have a function in stem cells and that, in general, exposure to Cd accelerated the onset and increased the severity of the observed phenotype. This suggested that the interaction between environmental and genetic factors plays an important role in tumor development in S. mediterranea. Therefore, we further focused on the synergistic effects of Cd exposure and p53 knockdown (KD) at the cellular and molecular levels. Cd also produced a specific proteomic landscape in homeostatic animals, with 172 proteins differentially expressed, 43 of which were downregulated. Several of these proteins have tumor suppressor function in human and other animals, namely Wilms Tumor 1 Associated Protein (WT1), Heat Shock Protein 90 (HSP90), Glioma Pathogenesis-Related Protein 1 (GLIPR1) and Matrix Metalloproteinase B (Smed-MMPB). Both Glipr1 and MmpB KD produced large outgrowths, epidermal lesions and epidermal blisters. The epidermal blisters that formed as a consequence of Smed-MmpB KD were populated by smedwi1+ cells, many of which were actively proliferating, while large outgrowths contained ectopically differentiated structures, such as photoreceptors, nervous tissue and a small pharynx. In conclusion, Smed-MmpB is a planarian TSG that prevents stem cell proliferation and differentiation outside the proper milieu.http://dmm.biologists.org/content/11/9/dmm032573PlanarianCadmiumCarcinogensMatrix-metalloproteinasesStem cellsTumor suppressor genes
collection DOAJ
language English
format Article
sources DOAJ
author Andromeda Van Roten
Amal Zohir Abo-Zeid Barakat
Annelies Wouters
Thao Anh Tran
Stijn Mouton
Jean-Paul Noben
Luca Gentile
Karen Smeets
spellingShingle Andromeda Van Roten
Amal Zohir Abo-Zeid Barakat
Annelies Wouters
Thao Anh Tran
Stijn Mouton
Jean-Paul Noben
Luca Gentile
Karen Smeets
A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
Disease Models & Mechanisms
Planarian
Cadmium
Carcinogens
Matrix-metalloproteinases
Stem cells
Tumor suppressor genes
author_facet Andromeda Van Roten
Amal Zohir Abo-Zeid Barakat
Annelies Wouters
Thao Anh Tran
Stijn Mouton
Jean-Paul Noben
Luca Gentile
Karen Smeets
author_sort Andromeda Van Roten
title A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
title_short A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
title_full A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
title_fullStr A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
title_full_unstemmed A carcinogenic trigger to study the function of tumor suppressor genes in Schmidtea mediterranea
title_sort carcinogenic trigger to study the function of tumor suppressor genes in schmidtea mediterranea
publisher The Company of Biologists
series Disease Models & Mechanisms
issn 1754-8403
1754-8411
publishDate 2018-09-01
description Planarians have been long known for their regenerative ability, which hinges on pluripotency. Recently, however, the planarian model has been successfully established for routine toxicological screens aimed to assess overproliferation, mutagenicity and tumorigenesis. In this study, we focused on planarian tumor suppressor genes (TSGs) and their role during chemically induced carcinogenic stress in Schmidtea mediterranea. Combining in silico and proteomic screens with exposure to human carcinogen type 1A agent cadmium (Cd), we showed that many TSGs have a function in stem cells and that, in general, exposure to Cd accelerated the onset and increased the severity of the observed phenotype. This suggested that the interaction between environmental and genetic factors plays an important role in tumor development in S. mediterranea. Therefore, we further focused on the synergistic effects of Cd exposure and p53 knockdown (KD) at the cellular and molecular levels. Cd also produced a specific proteomic landscape in homeostatic animals, with 172 proteins differentially expressed, 43 of which were downregulated. Several of these proteins have tumor suppressor function in human and other animals, namely Wilms Tumor 1 Associated Protein (WT1), Heat Shock Protein 90 (HSP90), Glioma Pathogenesis-Related Protein 1 (GLIPR1) and Matrix Metalloproteinase B (Smed-MMPB). Both Glipr1 and MmpB KD produced large outgrowths, epidermal lesions and epidermal blisters. The epidermal blisters that formed as a consequence of Smed-MmpB KD were populated by smedwi1+ cells, many of which were actively proliferating, while large outgrowths contained ectopically differentiated structures, such as photoreceptors, nervous tissue and a small pharynx. In conclusion, Smed-MmpB is a planarian TSG that prevents stem cell proliferation and differentiation outside the proper milieu.
topic Planarian
Cadmium
Carcinogens
Matrix-metalloproteinases
Stem cells
Tumor suppressor genes
url http://dmm.biologists.org/content/11/9/dmm032573
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