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首页> 外文期刊>Journal of Translational Medicine >Identification of two microRNA signatures in whole blood as novel biomarkers for diagnosis of nasopharyngeal carcinoma
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Identification of two microRNA signatures in whole blood as novel biomarkers for diagnosis of nasopharyngeal carcinoma

机译:鉴定全血两种microRNA签名作为新型生物标志物,用于诊断鼻咽癌

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摘要

Early diagnosis is critical to reduce the mortality caused by nasopharyngeal carcinoma (NPC). MicroRNAs (miRNAs) are dysregulated and play important roles in carcinogenesis. Therefore, this study aimed to identify diagnostically relevant circulating miRNA signatures in patients with NPC. Total RNA was extracted from whole blood samples obtained from 120 patients with NPC, 30 patients with head-neck tumors (HNT), and 30 healthy subjects (HSs), and examined by using a custom microarray. The expression levels of four miRNAs identified by using the microarray were validated with quantitative real-time reverse transcription polymerase chain reaction. The 120 patients with NPC and 30 HSs were randomly assigned to training group-1 and validation group-1, respectively. By using significance analysis of microarray (SAM), the specific miRNA expression profiles in whole blood from patients with NPC are obtained. By using lasso regression and adaptive boosting, a diagnostic signature was identified in training group-1, and its accuracy was verified in validation group-1. By using the same methods, another signature to distinguish patients with NPC from those with HNT and HSs was identified in training group-2 and confirmed in validation group-2. There were 117 differentially expressed miRNAs (upregulated and downregulated fold change ≥?1.5) between the patients with NPC and HSs, among which an 8-miRNA signature was identified with 96.43% sensitivity and 100% specificity [area under the curve (AUC)?=?0.995] to diagnose NPC in training group-1 and 86.11% sensitivity and 88.89% specificity (AUC?=?0.941) in validation group-1. Compared with traditional Epstein-Barr virus (EBV) seromarkers, this signature was more specific for NPC. Furthermore, a 16-miRNA signature to differentiate NPC from HNT and HS (HNT-HS) was established from 164 differentially expressed miRNAs, which diagnosed NPC and HNT-HS with 100% accuracy (AUC?=?1.000) in training group-2 and 87.04% (AUC?=?0.924) in validation group-2. The present study identified two miRNA signatures for the highly accurate diagnosis and differential diagnosis of patients with NPC from HSs and patients with HNT. The identified miRNAs might represent novel serological biomarkers and potential therapeutic targets for NPC.
机译:早期诊断对于降低鼻咽癌(NPC)引起的死亡率至关重要。 MicroRNAS(miRNA)在致癌物中进行了疑虑并发挥重要作用。因此,本研究旨在鉴定NPC患者的诊断相关循环miRNA签名。从120例NPC患者获得的全血样品中提取总RNA,30例头颈肿瘤(HNT)和30名健康受试者(HSS),并通过使用定制微阵列检查。通过使用微阵列鉴定的四种miRNA的表达水平验证了定量实时逆转录聚合酶链反应。随机分配120例NPC和30 HSS培训组-1和验证组-1。通过使用微阵列(SAM)的显着性分析,获得了NPC患者的全血中的特定miRNA表达谱。通过使用套索回归和自适应提升,在训练组-1中识别了诊断签名,并且在验证组-1中验证了其准确性。通过使用相同的方法,在训练组-2中鉴定了将患有NPC患者与HNT和HSS患者区分患者的签名,并在验证组-2中确认。 NPC和HSS患者之间有117个差异表达的miRNA(上调和下调和下调折叠变化≥≤1.5),其中鉴定了8- miRNA签名,鉴定了96.43%的敏感性和100%特异性[曲线下的区域(AUC)吗? =?0.995]诊断NPC在训练组-1和86.11%的敏感性和88.89%的特异性(AUC?= 0.941)中的验证组-1。与传统的Epstein-Barr病毒(EBV)血清瘤相比,这种签名更具体地对NPC。此外,从164个差异表达的miRNA建立了从HNT和HS(HNT-HS)中分化NPC的16-miRNA签名,其在训练组-2中诊断为NPC和HNT-HS的NPC和HNT-HS(AUC?=?1.000)验证组-2中的87.04%(AUC?= 0.924)。本研究确定了两种miRNA签名,用于高准确的HSS和HNT患者NPC患者的高精度诊断和鉴别诊断。确定的miRNA可以代表新型血清生物标志物和NPC的潜在治疗靶标。

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