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Molecular Biomarkers of Sessile Serrated Adenoma/Polyps

机译:无柄锯齿状腺瘤/息肉的分子生物标志物

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OBJECTIVES:Sessile serrated adenoma/polyps (SSA/Ps) contribute up to 30% of all colon cancers. There is considerable histological overlap between SSA/Ps and hyperplastic polyps. Inadequate consensus exists among pathologists, and no molecular biomarkers exist to differentiate these lesions with high accuracy. Lack of reliable diagnosis adversely affects clinical care. We previously defined a novel 7-gene panel by RNA sequencing that differentiates SSA/Ps from hyperplastic polyps. Here, we use the 7-gene panel as a molecular approach to differentiate SSA/Ps and HPs with higher sensitivity and specificity in a large sample set from a tertiary health care center.METHODS:Reverse transcription quantitative polymerase chain reaction of the 7-gene panel was performed on 223 formalin-fixed, paraffin-embedded serrated polyp and normal colon samples. We compare the sensitivity and specificity of the 7-gene panel with the BRAF and KRAS mutation incidence in differentiating SSA/Ps and HPs. We also evaluate the clinical data of patients with SSA/Ps showing high and low expression of the gene panel.RESULTS:The 7-gene RNA expression panel differentiates SSA/Ps and HPs with 89.2% sensitivity and 88.4% specificity. The gene panel outperforms BRAF mutation in identification of SSA/Ps. Clinical data suggest that expression of the 7-gene panel correlates with the development of SSA/Ps in the future.DISCUSSION:This study describes a novel 7-gene panel that identifies SSA/Ps with improved accuracy. Our data show that RNA markers of SSA/Ps advance the distinction of serrated lesions and contribute to the study of the serrated pathway to colon cancer.
机译:目的:无齿锯齿状腺瘤/息肉(SSA / Ps)占所有结肠癌的30%。 SSA / Ps和增生性息肉之间存在大量的组织学重叠。病理学家之间的共识不足,并且不存在分子生物学标记物可以高精度区分这些病变。缺乏可靠的诊断会对临床护理产生不利影响。我们之前通过RNA测序定义了一种新颖的7基因面板,可将SSA / Ps与增生性息肉区分开。在这里,我们使用7基因组作为分子方法来区分来自三级卫生保健中心的大量样品中具有更高灵敏度和特异性的SSA / Ps和HP。方法:7基因的逆转录定量聚合酶链反应在223个福尔马林固定,石蜡包埋的锯齿状息肉和正常结肠样本上进行了检测。我们比较了BRAF和KRAS突变发生率的7基因组在区分SSA / Ps和HPs中的敏感性和特异性。我们还评估了SSA / Ps患者基因组高表达和低表达的临床数据。结果:7基因RNA表达专家组以89.2%的敏感性和88.4%的特异性区分SSA / Ps和HPs。在鉴定SSA / Ps方面,基因组优于BRAF突变。临床数据表明,7基因专家组的表达与未来SSA / Ps的发展有关。讨论:本研究描述了一种新型的7基因专家组,其可以以更高的准确性鉴定SSA / Ps。我们的数据表明,SSA / Ps的RNA标记可促进锯齿状病变的区分,并有助于研究结肠癌的锯齿状途径。

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