CHK1 expression in gastric cancer is modulated by p53 and RB1/E2F1: Implications in chemo/radiotherapy response
Entity
UAM. Departamento de CirugíaPublisher
Nature Publishing GroupDate
2016-02-12Citation
10.1038/srep21519
Scientific Reports 6 (2016): 21519
ISSN
2045-2322DOI
10.1038/srep21519Funded by
This work was supported by Instituto de Salud Carlos III–Fondo de Investigación Sanitaria (PS09/1988 to ISP; PI11-00949, pI014-1495 and Feder Funds to RP); Comunidad Autónoma de Madrid-Universidad Autónoma de Madrid (CCG10-UAM/BIO-5871 to ISP); Fundación Leticia Castillejo Castillo and Ministerio de Ciencia e Innovación (SAF2012-30862 to RSP), Spain.Project
Gobierno de España. SAF2012-30862Editor's Version
http://dx.doi.org/10.1038/srep21519Subjects
Gastric cancer; Chk1; Radiotherapy; MedicinaRights
© 2016, Nature Publishing GroupAbstract
Radiation has a limited but relevant role in the adjuvant therapy of gastric cancer (GC) patients. Since Chk1 plays a critical function in cellular response to genotoxic agents, we aimed to analyze the role of Chk1 in GC as a biomarker for radiotherapy resistance. We analyzed Chk1 expression in AGS and MKN45 human GC cell lines by RT-QPCR and WB and in a small cohort of human patient’s samples. We demonstrated that Chk1 overexpression specifically increases resistance to radiation in GC cells. Accordingly, abrogation of Chk1 activity with UCN-01 and its expression with shChk1 increased sensitivity to bleomycin and radiation. Furthermore, when we assessed Chk1 expression in human samples, we found a correlation between nuclear Chk1 accumulation and a decrease in progression free survival. Moreover, using a luciferase assay we found that Chk1’s expression is controlled by p53 and RB/E2F1 at the transcriptional level. Additionally, we present preliminary data suggesting a posttranscriptional regulation mechanism, involving miR-195 and miR-503, which are inversely correlated with expression of Chk1 in radioresistant cells. In conclusion, Chk1/microRNA axis is involved in resistance to radiation in GC, and suggests Chk1 as a potential tool for optimal stratification of patients susceptible to receive adjuvant radiotherapy after surgery
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Google Scholar:Bargiela-Iparraguirre, J.
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Prado-Marchal, L.
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Fernandez-Fuente, M.
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Gutierrez- González, A.
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Moreno-Rubio, J.
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Muñoz-Fernandez, M.
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Sereno, M.
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Sanchez-Prieto, R.
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Perona, Rosario
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Sánchez Pérez, María Isabel
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