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EVI2B, ATP2A2, S100B, TM4SF3, and OLFM4 As Potential Prognostic Markers for Postoperative Taiwanese Colorectal Cancer Patients

机译:EVI2B,ATP2A2,S100B,TM4SF3和OLFM4作为台湾大肠癌术后患者的潜在预后指标

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Undetected micrometastasis may play a key role in the early relapse of colorectal cancer (CRC) patients. The aim of this study was to detect circulating tumor cells (CTCs) for predicting early relapse of CRC patients by a weighted enzymatic chip array (WEnCA) and analyze 15 candidate genes associated with CRC carcinogenesis. The genes of 105 postoperative CRC patients were analyzed by membrane array and direct sequencing. We constructed a WEnCA platform including five prognosis-related genes and analyzed the detection rate of WEnCA for CTCs in 30 clinically confirmed CRC relapse patients. Postoperative relapse was significantly correlated with gene overexpression, including EVI2B (p = 0.001, OR = 4.622), ATP2A2 (p = 0.006, OR = 4.688), S100B (p = 0.001, OR = 11.521), TM4SF3 (p = 0.001, OR = 6.756), and OLFM4 (p = 0.008, OR = 3.545). Using WEnCA (weighting score of each gene: 5 to EVI2B, 5 to ATP2A2, 12 to S100B, 7 to TM4SF3, and 4 to OLFM4), we could detect CTCs presenting these genotypes in relapsed CRC patients. The sensitivity, specificity, and accuracy were 94.7%, 93.5%, and 97%, respectively. The results of the present study suggest that EVI2B, ATP2A2, S100B, TM4SF3, and OLFM4 could be potential prognostic markers for CRC patients.
机译:未检测到的微转移可能在大肠癌(CRC)患者的早期复发中起关键作用。这项研究的目的是通过加权酶芯片阵列(WEnCA)检测循环肿瘤细胞(CTC)以预测CRC患者的早期复发,并分析15种与CRC致癌相关的候选基因。 105例术后CRC患者的基因通过膜阵列和直接测序分析。我们构建了一个包含5个与预后相关基因的WEnCA平台,并分析了30例临床确诊的CRC复发患者中WEnCA对四氯化碳的检出率。术后复发与基因过表达显着相关,包括EVI2B(p = 0.001,OR = 4.622),ATP2A2(p = 0.006,OR = 4.688),S100B(p = 0.001,OR = 11.521),TM4SF3(p = 0.001,OR) = 6.756)和OLFM4(p = 0.008,或= 3.545)。使用WEnCA(每个基因的权重得分:5对EVI2B,5对ATP2A2、12对S100B,7对TM4SF3和4对OLFM4),我们可以在复发的CRC患者中检测出呈现这些基因型的CTC。敏感性,特异性和准确性分别为94.7%,93.5%和97%。本研究的结果表明,EVI2B,ATP2A2,S100B,TM4SF3和OLFM4可能是CRC患者的潜在预后标志物。

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