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Correlation of APOBEC3 in tumor tissues with clinico-pathological features and survival from hepatocellular carcinoma after curative hepatectomy

机译:根治性肝切除术后肿瘤组织中APOBEC3与临床病理特征和肝细胞癌生存率的相关性

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摘要

Objective: This study aimed to evaluate the relationships between members of APOBEC3 in tumor tissues and hepatocellular carcinoma (HCC) aggressiveness and prognosis. Methods: Using the expression profile from Gene Expression Omnibus (GEO), we compared APOBEC3 expression between tumor and non-tumor tissues, and correlated this with clinico-pathological features and outcomes of HCC patients. Results: A3B, A3D, A3F and A3H were overexpressed in HCC tumor tissues compared to non-tumor tissues (all P≤0.001). Cox regression shown that A3G was negatively associated with overall survival of HCC patients (HR=2.277, 95% CI=1.324-3.915, P=0.033), in contrast, A3C level in tumor tissues might play a positive role in HCC overall survival (HR=0.364, 95% CI=0.182-0.727, P=0.004). Interestingly, A3F contributed to a poor disease-free survival of HCC (HR=3.383, 95% CI=1.249-9.715, P=0.017), while A3H may be a positive factor associated with HCC disease-free survival (HR=0.25, 95% CI=0.098-0.636, P=0.004). Cirrhosis, tumor size and intrahepatic metastasis were associated with HCC poor disease-free survival (HR=1.838, 95% CI=1.308-2.583, P<0.001; HR= 1.095, 95% CI=1.042-1.15, P<0.001 and HR=3.669, 95% CI=2.447-5.5, P<0.001; respectively). Logistic regression analysis indicated that up-regulation of A3F in tumor tissues promoted HCC vascular invasion, intrahepatic metastasis and AFP elevation (all P<0.05). In contrast, A3H might decrease these risks (all P<0.05). Conclusions: APOBEC3G and APOBEC3F might be risk factors for HCC development and survival, while APOBEC3C and APOBEC3H should play positive roles in HCC aggressiveness and prognosis. Further investigation for APOBEC3 mechanisms are needed in the future.
机译:目的:本研究旨在评估肿瘤组织中APOBEC3成员与肝细胞癌(HCC)侵袭性和预后的关系。方法:使用来自基因表达综合组织(GEO)的表达谱,我们比较了肿瘤和非肿瘤组织之间APOBEC3的表达,并将其与HCC患者的临床病理特征和预后相关。结果:与非肿瘤组织相比,HCC肿瘤组织中A3B,A3D,A3F和A3H过表达(均P≤0.001)。 Cox回归显示A3G与HCC患者的总生存呈负相关(HR = 2.277,95%CI = 1.324-3.915,P = 0.033),相反,肿瘤组织中的A3C水平可能对HCC的总生存起积极作用( HR = 0.364,95%CI = 0.182-0.727,P = 0.004)。有趣的是,A3F导致HCC无病生存率低(HR = 3.383,95%CI = 1.249-9.715,P = 0.017),而A3H可能是与HCC无病生存相关的积极因素(HR = 0.25, 95%CI = 0.098-0.636,P = 0.004)。肝硬化,肿瘤大小和肝内转移与HCC不良无病生存率相关(HR = 1.838,95%CI = 1.308-2.583,P <0.001; HR = 1.095,95%CI = 1.042-1.15,P <0.001和HR = 3.669,95%CI = 2.447-5.5,P <0.001;)。 Logistic回归分析表明,肿瘤组织中A3F的上调促进了HCC血管浸润,肝内转移和AFP升高(所有P <0.05)。相反,A3H可能会降低这些风险(所有P <0.05)。结论:APOBEC3G和APOBEC3F可能是肝癌发生和生存的危险因素,而APOBEC3C和APOBEC3H在肝癌的侵袭性和预后中应发挥积极作用。将来需要进一步研究APOBEC3机制。

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