Cryptosporidium parvum-induced ileo-caecal adenocarcinoma and Wnt signaling in a mouse model

被引:34
作者
Benamrouz, Sadia [1 ,2 ]
Conseil, Valerie [1 ,2 ]
Chabe, Magali [2 ,3 ]
Praet, Marleen [4 ]
Audebert, Christophe [5 ,6 ]
Blervaque, Renaud [5 ,7 ]
Guyot, Karine [2 ]
Gazzola, Sophie [2 ]
Mouray, Anthony [8 ]
Chassat, Thierry [8 ]
Delaire, Baptiste [9 ]
Goetinck, Nathalie [10 ]
Gantois, Nausicaa [2 ]
Osman, Marwan [2 ,11 ]
Slomianny, Christian [12 ]
Dehennaut, Vanessa [13 ]
Lefebvre, Tony [13 ]
Viscogliosi, Eric [2 ]
Cuvelier, Claude [4 ]
Dei-Cas, Eduardo [2 ,10 ]
Creusy, Colette [9 ]
Certad, Gabriela [2 ]
机构
[1] Univ Lille Nord France, Univ Catholique Lille, Fac Libre Sci & Technol Lille, F-59020 Lille, France
[2] Univ Lille Nord France, CNRS UMR 8402, Ctr Infect & Immun Lille, Inst Pasteur Lille,INSERM U1019, F-59021 Lille, France
[3] Univ Lille Nord France, Fac Pharm, F-59021 Lille, France
[4] Univ Ghent, Acad Dept Pathol, B-9000 Ghent, Belgium
[5] Inst Pasteur, PEGASE Biosci, F-59021 Lille, France
[6] Gene Diffus, F-59501 Douai, France
[7] Univ Lille Nord France, Ctr Infect & Immun Lille, Inst Pasteur Lille, INSERM U1019,CNRS UMR 8404, F-59021 Lille, France
[8] Inst Pasteur, F-59021 Lille, France
[9] Grp Hosp Univ Catholique Lille, Serv Anat & Cytol Pathol, F-59020 Lille, France
[10] Univ Lille Nord France, CHRU Lille, F-59000 Lille, France
[11] Univ Libanaise, Ctr AZM Rech Biotechnol & Ses Applicat, Lab Microbiol Sante & Environm, Tripoli, Lebanon
[12] Univ Lille 1, Lab Physiol Cellulaire, INSERM, U1003, F-59655 Villeneuve Dascq, France
[13] Univ Lille 1, Unite Glycobiol Struct & Fonct, UMR CNRS 8576, IFR 147, F-59650 Villeneuve Dascq, France
关键词
SCID mouse model; Cryptosporidiosis; Wnt pathway; Cytoskeleton; Digestive cancer; BETA-CATENIN; FULMINANT CRYPTOSPORIDIOSIS; COLON CARCINOGENESIS; COLORECTAL-CANCER; GENE-EXPRESSION; MUTATIONS; CELLS; NEOPLASIA; INFECTION; MEMBRANE;
D O I
10.1242/dmm.013292
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Cryptosporidium species are apicomplexan protozoans that are found worldwide. These parasites constitute a large risk to human and animal health. They cause self-limited diarrhea in immunocompetent hosts and a life-threatening disease in immunocompromised hosts. Interestingly, Cryptosporidium parvum has been related to digestive carcinogenesis in humans. Consistent with a potential tumorigenic role of this parasite, in an original reproducible animal model of chronic cryptosporidiosis based on dexamethasone-treated or untreated adult SCID mice, we formerly reported that C. parvum (strains of animal and human origin) is able to induce digestive adenocarcinoma even in infections induced with very low inoculum. The aim of this study was to further characterize this animal model and to explore metabolic pathways potentially involved in the development of C. parvum-induced ileo-caecal oncogenesis. We searched for alterations in genes or proteins commonly involved in cell cycle, differentiation or cell migration, such as beta-catenin, Apc, E-cadherin, Kras and p53. After infection of animals with C. parvum we demonstrated immunohistochemical abnormal localization of Wnt signaling pathway components and p53. Mutations in the selected loci of studied genes were not found after high-throughput sequencing. Furthermore, alterations in the ultrastructure of adherens junctions of the ileo-caecal neoplastic epithelia of C. parvum-infected mice were recorded using transmission electron microscopy. In conclusion, we found for the first time that the Wnt signaling pathway, and particularly the cytoskeleton network, seems to be pivotal for the development of the C. parvum-induced neoplastic process and cell migration of transformed cells. Furthermore, this model is a valuable tool in understanding the host-pathogen interactions associated with the intricate infection process of this parasite, which is able to modulate host cytoskeleton activities and several host-cell biological processes and remains a significant cause of infection worldwide.
引用
收藏
页码:693 / 700
页数:8
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