首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Combination of plasma microRNAs with serum CA19-9 for early detection of pancreatic cancer
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Combination of plasma microRNAs with serum CA19-9 for early detection of pancreatic cancer

机译:血浆microRNA与血清CA19-9的结合用于胰腺癌的早期检测

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摘要

This study was performed to identify plasma microRNAs (miRNAs) as diagnostic biomarkers for pancreatic cancer (PCa) and to assess their supplementary role with serum CA19-9 in early identification of tumors. Plasma RNAs were extracted from 140 PCa patients, 111 chronic pancreatitis (CP) patients and 68 normal controls, and the relative abundances of seven miRNAs (miR-16, 21, 155, 181a, 181b, 196a and 210) were measured using real-time PCR. Their diagnostic utility for PCa and correlation with clinical characteristics were analyzed. All seven miRNAs were significantly aberrantly upregulated in the PCa group compared with both the CP and normal groups, between which only four miRNAs (miR-155, 181a, 181b and 196a) were significantly different. Logistic modeling proved that only miR-16 and miR-196a possessed an independent role in discriminating PCa from normal and CP. Furthermore, after including serum CA19-9 in the logistic model, the combination of miR-16, miR-196a and CA19-9 was more effective for discriminating PCa from non-PCa (normal+CP) (AUC-ROC, 0.979; sensitivity, 92.0%; specificity, 95.6%), and for discriminating PCa from CP (AUC-ROC, 0.956; sensitivity, 88.4%; specificity, 96.3%) compared with the miRNA panel (miR-16+miR-196a) or CA19-9 alone. Most significantly, the combination was effective at identification of tumors in Stage 1 (85.2%). In conclusion, plasma miRNAs were effective for distinguishing PCa from non-PCa (normal+CP). The combination of miR-16, miR-196a and CA19-9 was more effective for PCa diagnosis, especially in early tumor screening.
机译:进行这项研究以鉴定血浆microRNA(miRNA)作为胰腺癌(PCa)的诊断生物标志物,并评估它们与血清CA19-9在肿瘤的早期鉴定中的补充作用。从140例PCa患者,111例慢性胰腺炎(CP)患者和68例正常对照中提取血浆RNA,并使用real-time方法测量了7种miRNA(miR-16、21、155、181a,181b,196a和210)的相对丰度。时间PCR。分析了它们对PCa的诊断效用及其与临床特征的相关性。与CP组和正常组相比,PCa组中的所有7个miRNA均明显异常上调,其中只有4个miRNA(miR-155、181a,181b和196a)显着不同。逻辑模型证明,只有miR-16和miR-196a在区分PCa与正常和CP方面具有独立的作用。此外,在逻辑模型中加入血清CA19-9后,miR-16,miR-196a和CA19-9的组合更能有效区分PCa和非PCa(正常+ CP)(AUC-ROC,0.979;敏感性) ,92.0%;特异性为95.6%),以及与miRNA小组(miR-16 + miR-196a)或CA19- 9个。最重要的是,该组合可有效识别第1阶段的肿瘤(85.2%)。总之,血浆miRNA可有效区分PCa与非PCa(正常+ CP)。 miR-16,miR-196a和CA19-9的组合对PCa诊断更有效,尤其是在早期肿瘤筛查中。

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