| Literature DB >> 25497869 |
Vincenza Leone1, Angelo Ferraro1, Filippo Schepis2, Antonella Federico1, Romina Sepe1, Claudio Arra3, Concetta Langella1, Giuseppe Palma4, Carlo De Lorenzo2, Giancarlo Troncone5, Valeria Masciullo6, Giovanni Scambia6, Alfredo Fusco1, Pierlorenzo Pallante7.
Abstract
We have previously reported that the expression of the CL2/CCDC80 gene is downregulated in human papillary thyroid carcinomas, particularly in follicular variants. We have also reported that the restoration of CL2/CCDC80 expression reverted the malignant phenotype of thyroid carcinoma cell lines and that CL2/CCDC80 positively regulated E-cadherin expression, an ability that likely accounts for the role of the CL2/CCDC80 gene in thyroid cancer progression. In order to validate the tumour suppressor role of the CL2/CCDC80 gene in thyroid carcinogenesis we generated cl2/ccdc80 knock-out mice. We found that embryonic fibroblasts from cl2/ccdc80(-/-) mice showed higher proliferation rate and lower susceptibility to apoptosis. Furthermore, cl2/ccdc80(-/-) mice developed thyroid adenomas and ovarian carcinomas. Finally, ret/PTC1 transgenic mice crossed with the cl2/ccdc80 knock-out mice developed more aggressive thyroid carcinomas compared with those observed in the single ret/PTC1 transgenic mice. Together, these results indicate CL2/CCDC80 as a putative tumour suppressor gene in human thyroid carcinogenesis.Entities:
Keywords: Carcinoma; Knock-out mice; Ovary; Thyroid; cl2/dro1/ccdc80
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Year: 2014 PMID: 25497869 DOI: 10.1016/j.canlet.2014.12.010
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679