大肠癌中存活素 mRNA(BIRC5)表达的临床意义

Andrey V. Orekhva, E. A. Shlyakhtunov, V. M. Semenov, I. Zhiltsov, A. V. Erushevich, G. M. Shappo, Ya. N. Lyakh, Alina V. Orekhva
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All patients underwent complete tumor removal (radical surgery – 93.6 %), cytoreductive – 6.4 %).A high level of survivin (BIRC5) mRnA expression was detected in colorectal adenocarcinoma in comparison with adenomas (pMann–whitney < 0.001) M ± SD (1.678 ± 2.45 and 0.023 ± 0.07). In the study and observation group, the expression of survivin mRnA (BIRC5) in CTCs both before surgery M ± SD (1.175 ± 1.33 and 0.052 ± 0.11) and after 3 months M ± SD (1.015 ± 0.93 and 0.018 ± 0.002) was significantly different (pMann–whitney <0.001).During adjuvant chemotherapy, a decrease in the level of survivin expression in CTCs was observed (p 9 months after surgery, CTCs remain in the bloodstream even despite adjuvant chemotherapy (p = 0.015 and p = 0.012). Overexpression of survivin in CTCs before surgery correlates with damage to regional lymph nodes (p = 0.03, r = 0.21), stage of the tumor process (p = 0.01, r = 0.25), degree of tumor differentiation (p = 0.03, r = 0.21). 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摘要

目的评估循环肿瘤细胞(CTCs)和结直肠癌(CRC)肿瘤材料中存活素(BIRC5)mRnA表达的临床意义。本研究按照连续前瞻性非随机研究的原则组织。采用 RT-pCR 方法测定 CTCs 和肿瘤材料中存活素(BIRC5)mRnA 的表达。该研究包括 130 名患者(研究组--109 名结直肠癌患者,观察组--21 名结肠腺瘤患者)。与腺瘤相比,在结直肠腺癌中检测到高水平的存活素(BIRC5)mRnA表达(pMann-whitney < 0.001)M ± SD(1.678 ± 2.45 和 0.023 ± 0.07)。在研究组和观察组中,手术前M±SD(1.175±1.33和0.052±0.11)和3个月后M±SD(1.015±0.93和0.018±0.002)的CTC中survivin mRnA(BIRC5)的表达均有显著差异(pMann-whitney <0.001).在辅助化疗期间,观察到 CTC 中存活素表达水平下降(p 手术 9 个月后,尽管进行了辅助化疗,CTC 仍留在血液中(p = 0.015 和 p = 0.012)。手术前 CTCs 中 survivin 的过表达与区域淋巴结的损伤(p = 0.03,r = 0.21)、肿瘤进程分期(p = 0.01,r = 0.25)、肿瘤分化程度(p = 0.03,r = 0.21)相关。术后9个月CTCs中survivin的过表达显著影响患者的无复发生存率HR(95 % CI HR)=3.1(95 % CI 1.56-6.08,p = 0.0012)和总生存率HR(95 % CI HR)=6.8(95 % CI 2.65-17.33,p = 0.0001)。生存素 mRnA 在结直肠癌中的过表达是该病的一个负性预后因素,直接取决于肿瘤累及区域淋巴结、疾病分期、肿瘤分化程度,促进疾病复发的发展,可用于诊断极小残留病(MRD)和评估患者总生存期的预后。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical significance of survivin mRNA expression (BIRC5) in colorectal cancer
Aim. To evaluate the clinical significance of survivin (BIRC5) mRnA expression in circulating tumor cells (CTCs) and tumor material from colorectal cancer (CRC).Materials and methods. The study was organized according to the principle of a continuous prospective non-randomized study. The expression of survivin (BIRC5) mRnA in CTCs and tumor material was determined using RT-pCR.Results. The study included 130 patients (study group – 109 patients with colorectal cancer and observation group – 21 patients with colon adenomas). All patients underwent complete tumor removal (radical surgery – 93.6 %), cytoreductive – 6.4 %).A high level of survivin (BIRC5) mRnA expression was detected in colorectal adenocarcinoma in comparison with adenomas (pMann–whitney < 0.001) M ± SD (1.678 ± 2.45 and 0.023 ± 0.07). In the study and observation group, the expression of survivin mRnA (BIRC5) in CTCs both before surgery M ± SD (1.175 ± 1.33 and 0.052 ± 0.11) and after 3 months M ± SD (1.015 ± 0.93 and 0.018 ± 0.002) was significantly different (pMann–whitney <0.001).During adjuvant chemotherapy, a decrease in the level of survivin expression in CTCs was observed (p 9 months after surgery, CTCs remain in the bloodstream even despite adjuvant chemotherapy (p = 0.015 and p = 0.012). Overexpression of survivin in CTCs before surgery correlates with damage to regional lymph nodes (p = 0.03, r = 0.21), stage of the tumor process (p = 0.01, r = 0.25), degree of tumor differentiation (p = 0.03, r = 0.21). Overexpression of survivin in CTCs 9 months after surgery significantly affects relapse-free survival HR (95 % CI HR) = 3.1 (95 % CI 1.56–6,08, p = 0.0012) and overall survival of patients HR (95 % CI HR) =6.8 (95 % CI 2.65–17.33, p = 0.0001).Conclusions. Overexpression of survivin mRnA in colorectal cancer is a negative prognosis factor for the disease and directly depends on the tumor involvement of regional lymph nodes, the stage of the disease, degree of tumor differentiation, promoting the development of disease relapse, and can be used to diagnose minimal residual disease (MRD) and assess the prognosis of overall patient survival.
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