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Prognostic impact of telomeric repeat-containing RNA expression on long-term oncologic outcomes in colorectal cancer

机译:端粒重复RNA表达对结直肠癌长期肿瘤成果的预后影响

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Telomeres are transcribed into long, noncoding telomeric repeat-containing RNAs (TERRA) that have been implicated in the regulation of telomerase, the enzyme that lengthens telomeres, in heterochromatin formation at telomeres, and in telomere stability. This study aimed to evaluate the correlation between TERRA expression and long-term oncologic outcomes in colorectal cancer (CRC). We evaluated 18p TERRA expression and telomere length using quantitative real-time PCR in 60 patients who underwent surgical resection for CRC between June 2008 and November 2010. Patients were grouped according to 18p TERRA expression, with 29 (48.3%) and 31 (51.7%) patients in the low and high TERRA expression groups, respectively. The median follow-up period was 80 months (range 2–103). The 18p TERRA expression was marginally significantly associated with preoperative carcinoembryonic antigen (CEA; P = .082) and was significantly associated with telomere length ( P .05). Multivariate analysis revealed that preoperative CEA (hazard ratio [HR], 2.728; 95% confidence interval [CI], 0.832–8.944, P = .098) and 18p TERRA expression (HR, 0.113; 95% CI, 0.011–1.126, P = .071) were marginally significant independent prognostic factors for overall survival (OS), whereas preoperative CEA (HR, 4.254; 95% CI, 1.394–12.985, P = .011) and 18p TERRA expression (HR, 0.108; 95% CI, 0.011–1.037, P = .054) were significant independent prognostic factors for disease-free survival (DFS). According to our prognostic model with 2 prognostic factors, the OS and DFS rate increased to 76.2% and 80.63%, respectively, in patients with high 18p TERRA expression and CEA levels ≤5 ( P = .178, P = .057, respectively). 18p TERRA expression was marginally significantly associated with preoperative CEA and significantly associated with telomere length, rendering it a potential prognostic factor for long-term oncologic outcomes in CRC.
机译:端粒被转录为长期的非编码的端粒重复的RNA(Terra),该含有含有端粒酶的调节,延长端粒的酶的酶,在端粒的形状蛋白形成中,并以端粒稳定性。本研究旨在评估结肠直肠癌(CRC)中Terra表达与长期肿瘤结果的相关性。我们在2008年6月和2010年11月期间接受了CRC手术切除的60名患者的定量实时PCR评估了18P Terra表达和端粒长度。根据18P的Terra表达进行分组,29%(48.3%)和31(51.7%)进行分组)分别为低层和高层表达组的患者。中位后续期间为80个月(2-103级)。 18P Terra表达与术前癌症抗原(CEA; P = .082)略微明显相关,并且与端粒长度显着相关(P <.05)。多变量分析显示,术前CEA(危害比[HR],2.728; 95%置信区间[CI],0.832-8.944,P = .098)和18P Terra表达(HR,0.113; 95%CI,0.011-1.126,P = .071)对整体存活(OS)进行略微显着的独立预后因素,而术前CEA(HR,4.254; 95%CI,1.394-12.985,P = .011)和18P Terra表达(HR,0.108; 95%CI) ,0.011-1.037,p = .054)是无疾病存活(DFS)的显着独立的预后因素。根据我们的预后模型,具有2个预后因素的预后模型,OS和DFS率分别增加到高18P滴度表达和CEA水平≤5(P = .178,P = .057)的患者中增加到76.2%和80.63% 。 18P Terra表达与术前CEA有明显明显明显,与端粒长度显着相关,使其具有CRC中长期肿瘤结果的潜在预后因素。

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