Publication: Amplification of D22S283 as a favorable prognostic indicator in liver fluke related cholangiocarcinoma
Issued Date
2006-07-21
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ISSN
10079327
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2-s2.0-33746877567
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Mahidol University
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SCOPUS
Bibliographic Citation
World Journal of Gastroenterology. Vol.12, No.27 (2006), 4338-4344
Suggested Citation
Jongkonnee Thanasai, Temduang Limpaiboon, Patcharee Jearanaikoon, Vajarabhongsa Bhudhisawasdi, Narong Khuntikeo, Banchob Sripa, Masanao Miwa Amplification of D22S283 as a favorable prognostic indicator in liver fluke related cholangiocarcinoma. World Journal of Gastroenterology. Vol.12, No.27 (2006), 4338-4344. doi:10.3748/wjg.v12.i27.4338 Retrieved from: https://repository.li.mahidol.ac.th/handle/20.500.14594/23694
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Title
Amplification of D22S283 as a favorable prognostic indicator in liver fluke related cholangiocarcinoma
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Abstract
Aim: To analyze the DNA copy number of target genes NF2, TIMP3, ST13, TOB2, BIK, and TP and the reference microsatellite markers D22S283, D22S423, and D22S274 mapped on 22q12-qter in liver fluke related cholangiocarcinoma (CCA) and define its correlation with clinical parameters. Methods: Quantitative real time PCR (qPCR) was used for determining allelic imbalances in 65 liver fluke related CCA tissues. Statistical correlations between allelic imbalances and clinicopathological parameters, i.e. age, sex, tumor stage, histological type, blood vessel invasion, nerve invasion and lymphatic invasion were evaluated by means of the χ2test. Cox regression analysis was used for determining patient's survival. Results: Amplifications of the TP (22q13.33), TOB2 (22q13.2-13.31), D22S283 (22q12.3), TIMP3 (22q12.3) and NF2 (22q12.2) were found in 35 (53.8%), 28 (43.1%), 27 (41.5%), 24 (36.9%), and 24 (36.9%), respectively. Losses at the D22S423 (22q13.1-13.2) and BIK (22q13.31) were detected in 26 (40%) and 23 (35.4%), respectively. Significant correlations were observed between lymphatic invasion and allelic losses of BIK (P = 0.025) and D22S283 (P = 0.041). Univariate and multivariate Cox regression analysis revealed D22S283 amplification as an independent predictor of good prognosis (P = 0.006, death hazard ratio = 0.411, 95% CI = 0.217-0.779) and blood vessel invasion as an independent poor prognostic factor (P = 0.042, death hazard ratio = 1.911, 95% CI = 1.022-3.571) in CCA patients. Conclusion: This study provides evidence for the involvement of gene amplification and deletion on chromosome 22q in liver fluke related CCA. This is the first report of D22S283 amplification as an independent indicator of favorable prognosis in liver fluke related CCA. © 2006 The WJG Press. All rights reserved.