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循环 Epstein-Barr 病毒 microRNAs miR-BART7 和 miR-BART13 作为鼻咽癌诊断和治疗的生物标志物。

Circulating Epstein-Barr virus microRNAs miR-BART7 and miR-BART13 as biomarkers for nasopharyngeal carcinoma diagnosis and treatment.

机构信息

State Key Laboratory for Emerging Infectious Diseases, Department of Microbiology and Research Centre of Infection and Immunology, The University of Hong Kong, Hong Kong SAR, People's Republic of China.

出版信息

Int J Cancer. 2015 Mar 1;136(5):E301-12. doi: 10.1002/ijc.29206. Epub 2014 Sep 18.

Abstract

More than 75% of nasopharyngeal carcinoma (NPC) patients have already developed local or regional spread at diagnosis, which hampers effective treatment and results in a poor prognosis. It is essential to characterize more sensitive and specific biomarkers for screening of high risk individuals and assessment of NPC treatment effectiveness. NPC is an Epstein-Barr virus (EBV) associated tumor in which only a few viral proteins but more than 20 BamHI A rightward transcripts (BART) microRNAs are detected, at abundant levels. We hypothesized that these BART microRNAs may be novel biomarkers for NPC. Systematic analysis of EBV BART microRNA expression profiles in EBV latently infected Mutu I and Mutu III cell lines, EBV-harboring NPC and noncancerous NP cells found that miR-BART3, miR-BART7 and miR-BART13 microRNAs are highly expressed and regularly secreted into the extracellular environment of NPC cells. These BART microRNAs were evaluated for used as potential NPC biomarkers. Analysis of plasma specimens obtained from NPC patients (n = 89), and healthy (n = 28) and non-NPC tumor patient controls (n = 18) found levels of both miR-BART7 and miR-BART13, but not miR-BART3, to be distinctly presence among NPC patients, with elevated levels being particularly apparent among patients with advanced disease. Receiver operating characteristic curve analysis combining miR-BART7 and miR-BART13 levels produces a 90% predictive value for the presence of NPC. Analysis of 41 NPC patients before and after radiotherapy showed that miR-BART7 and miR-BART13, but not miR-BART3, were diminished after treatment. These results indicate that EBV microRNAs, miR-BART7 and miR-BART13, may constitute useful new serological biomarkers for diagnosis of NPC and prediction of treatment efficacy.

摘要

超过 75%的鼻咽癌 (NPC) 患者在诊断时已经出现局部或区域扩散,这阻碍了有效的治疗并导致预后不良。因此,有必要寻找更敏感和特异的生物标志物,用于高危人群的筛查和 NPC 治疗效果的评估。NPC 是一种 EBV 相关肿瘤,其中只有少数病毒蛋白,但有超过 20 个 BamHI A 右向转录物 (BART) 微 RNA 被检测到,且表达水平丰富。我们假设这些 BART 微 RNA 可能是 NPC 的新型生物标志物。对 EBV 潜伏感染的 Mutu I 和 Mutu III 细胞系、EBV 携带的 NPC 和非癌性 NP 细胞中的 EBV BART 微 RNA 表达谱进行系统分析发现,miR-BART3、miR-BART7 和 miR-BART13 微 RNA 高度表达,并经常分泌到 NPC 细胞的细胞外环境中。这些 BART 微 RNA 被评估为 NPC 的潜在生物标志物。对 89 名 NPC 患者、28 名健康对照者和 18 名非 NPC 肿瘤患者的血浆标本进行分析发现,miR-BART7 和 miR-BART13 的水平在 NPC 患者中明显存在,而 miR-BART3 的水平则不存在,疾病晚期患者的水平升高尤为明显。结合 miR-BART7 和 miR-BART13 水平的受试者工作特征曲线分析对 NPC 的存在具有 90%的预测价值。对 41 名 NPC 患者放疗前后的分析表明,miR-BART7 和 miR-BART13 在治疗后下降,但 miR-BART3 则没有。这些结果表明,EBV 微 RNA,miR-BART7 和 miR-BART13,可能构成有用的 NPC 诊断和治疗效果预测的新型血清学生物标志物。

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