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Published in: Discover Oncology 3/2018

01-06-2018 | Original Paper

Thyroid Hormone Promotes β-Catenin Activation and Cell Proliferation in Colorectal Cancer

Authors: Yee-Shin Lee, Yu-Tang Chin, Ya-Jung Shih, André Wendindondé Nana, Yi-Ru Chen, Han-Chung Wu, Yu-Chen S. H. Yang, Hung-Yun Lin, Paul J. Davis

Published in: Discover Oncology | Issue 3/2018

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Abstract

Thyroid hormone status has long been implicated in cancer development. Here we investigated the role of thyroxine (T4) in colorectal cancer cell lines HCT 116 (APC wild type) and HT-29 (APC mutant), as well as the primary cultures of cancer cells derived from patients. Cell proliferation was evaluated with standard assay and proliferation marker expression. β-Catenin activation was examined according to nuclear β-catenin accumulation and β-catenin target gene expression. The results showed that T4 increased colorectal cancer cell proliferation while cell number and viability were elevated by T4 in both established cell lines and primary cells. Moreover, the transcriptions of proliferative genes PCNA, CCND1, and c-Myc were enhanced by T4 in the primary cells. T4 induced nuclear β-catenin accumulation, as well as high cyclin D1 and c-Myc levels compared to the untreated cells. In addition, the β-catenin-directed transactivation of CCND1 and c-Myc promoters was also upregulated by T4. CTNNB1 transcription was raised by T4 in HCT 116, but not in HT-29, while the boosted β-catenin levels were observed in both. Lastly, the T4-mediated gene expression could be averted by the knockdown of β-catenin. These results suggested that T4 promotes β-catenin activation and cell proliferation in colorectal cancer, indicating that an applicable therapeutic strategy should be considered.
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Metadata
Title
Thyroid Hormone Promotes β-Catenin Activation and Cell Proliferation in Colorectal Cancer
Authors
Yee-Shin Lee
Yu-Tang Chin
Ya-Jung Shih
André Wendindondé Nana
Yi-Ru Chen
Han-Chung Wu
Yu-Chen S. H. Yang
Hung-Yun Lin
Paul J. Davis
Publication date
01-06-2018
Publisher
Springer US
Published in
Discover Oncology / Issue 3/2018
Print ISSN: 1868-8497
Electronic ISSN: 2730-6011
DOI
https://doi.org/10.1007/s12672-018-0324-y

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