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Identification of circulating miRNA profiles that distinguish malignant pleural mesothelioma from lung adenocarcinoma

机译:鉴别区分恶性胸膜间皮瘤和肺腺癌的循环miRNA图谱

摘要

Accurate diagnosis of malignant pleura mesothelioma (MPM) is challenging. Differential diagnosis of MPM versus lung adenocarcinoma (AD) is particularly difficult, yet clinically important since the two neoplasias call for different treatment approaches. Circulating miRNA-profiling to identify miRNAs that can be used to distinguish MPM from AD has not been reported. We conducted a wide screening study of miRNA profiles in serum pools of MPM patients (N = 11), AD patients (N = 36), and healthy subjects (N = 45) to identify non-invasive biomarkers for differential diagnosis of MPM and AD, using deep sequencing. Sequencingdetected up to 300 known miRNAs and up to 25 novel miRNAs species in the serum samples. Among known miRNAs, 7 were upregulated in MPM and 12 were upregulated in AD compared to healthy controls. Of these, eight were distinctive for AD and three were unique for MPM. Direct comparison of the miRNA profiles for MPM and AD revealed differences in miRNA levels that could be useful for differential diagnosis. No differentially expressed novel miRNAs were found. Further bioinformatics analysis indicated that three upregulated miRNAs in MPM are associated with the p38 pathway. There are unique alterations in serum miRNAs in MPM and AD compared to healthy controls, as well as differences between MPM and AD profiles. Differing miRNA levels between MPM and AD may be useful for differential diagnosis. A potential association to p38 pathway of three upregulated miRNAs in MPM was revealed.
机译:恶性胸膜间皮瘤(MPM)的准确诊断具有挑战性。 MPM与肺腺癌(AD)的鉴别诊断特别困难,但由于两个肿瘤形成需要不同的治疗方法,因此具有重要的临床意义。尚未进行循环miRNA分析以鉴定可用于区分MPM和AD的miRNA。我们对MPM患者(N = 11),AD患者(N = 36)和健康受试者(N = 45)的血清库中的miRNA谱进行了广泛的筛选研究,以鉴定非侵入性生物标志物,以区别诊断MPM和AD ,使用深度排序。测序可在血清样品中检测到多达300种已知的miRNA和多达25种新的miRNA。与健康对照组相比,已知的miRNA中有7个在MPM中上调,在12个在AD中上调。其中,八个对于广告是独特的,而三个对于MPM是独特的。对MPM和AD的miRNA谱图的直接比较显示,miRNA水平的差异可能对鉴别诊断有用。没有发现差异表达的新型miRNA。进一步的生物信息学分析表明,MPM中的三个上调的miRNA与p38途径相关。与健康对照组相比,MPM和AD中的血清miRNA有独特的变化,以及MPM和AD谱之间的差异。 MPM和AD之间不同的miRNA水平可能有助于鉴别诊断。揭示了与MPM中三个上调的miRNA的p38途径的潜在关联。

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