首页> 外文期刊>World Journal of Gastroenterology >Amplification of D22S283 as a favorable prognostic indicator in liver fluke related cholangiocarcinoma.
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Amplification of D22S283 as a favorable prognostic indicator in liver fluke related cholangiocarcinoma.

机译:D22S283的扩增作为肝吸虫相关胆管癌的有利预后指标。

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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 chi2 test. 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.
机译:目的:分析靶基因NF2,TIMP3,ST13,TOB2,BIK和TP的DNA拷贝数,以及映射在肝吸虫相关胆管癌(CCA)中22q12-qter上的参考微卫星标记D22S283,D22S423和D22S274,并对其定义与临床参数的相关性。方法:实时定量PCR(qPCR)用于确定65例肝吸虫相关CCA组织中的等位基因失衡。等位基因失衡与临床病理参数之间的统计相关性,即年龄,性别,肿瘤分期,组织学类型,血管侵袭,神经侵袭和淋巴管侵袭,通过chi2检验进行评估。考克斯回归分析用于确定患者的生存。结果:在35(53.8%)中发现了TP(22q13.33),TOB2(22q13.2-13.31),D22S283(22q12.3),TIMP3(22q12.3)和NF2(22q12.2)的扩增, 28(43.1%),27(41.5%),24(36.9%)和24(36.9%)。在D22S423(22q13.1-13.2)和BIK(22q13.31)处分别检测到26(40%)和23(35.4%)的损失。观察到淋巴管浸润和BIK(P = 0.025)和D22S283(P = 0.041)的等位基因丧失之间存在显着相关性。单因素和多因素Cox回归分析显示D22S283扩增是预后良好的独立预测因子(P = 0.006,死亡危险比= 0.411,95%CI = 0.217-0.779),而血管浸润是独立的不良预后因素(P = 0.042, CCA患者的死亡风险比= 1.911,95%CI = 1.022-3.571)。结论:本研究为肝吸虫相关CCA中22q染色体基因的扩增和缺失提供了证据。这是D22S283扩增作为肝吸虫相关CCA预后良好的独立指标的首次报道。

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