肿瘤蛋白基因组学鉴定尿液S100A9和GRN是早期诊断肝细胞癌的潜在组合生物标志物

Chun-Hao Huang , Chao-Jen Kuo , Shih-Shin Liang , Shu-Wen Chi , Edward Hsi , Chi-Chao Chen , King-Teh Lee , Shyh-Horng Chiou
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引用次数: 32

摘要

肝细胞癌(HCC)是肝癌的主要类型,由于其侵袭性和经常发现较晚,是最致命的癌症之一。因此,识别早期诊断标记物的可能性可能会带来重大益处。尿液尤其成为生物标志物发现中最具吸引力的体液之一,因为它可以大量非侵入性地获得,并且与其他体液相比具有稳定性。为了确定HCC早期诊断的潜在蛋白质生物标志物,我们利用纳米液相色谱-串联质谱(nanoLC-MS /MS)和稳定同位素二甲基标记,通过鸟枪蛋白质组学研究了HCC患者和正常对照(n = 44)尿液中的蛋白质表达谱。我们系统地绘制了91种差异表达蛋白(p <0.05),包括8个下调的微管蛋白和83个上调的微管蛋白参与信号和炎症反应。通过蛋白质组学、基因组学和转录组学分析进一步整合蛋白质基因组学方法,发现S100A9和GRN共扩增(p <0.001)和共表达(p <0.01)。此外,我们还发现S100A9或GRN的扩增与HCC患者的低生存率相关,并且它们的共同扩增也比单个扩增的预后总生存率差。我们的研究结果表明,尿液S100A9和GRN作为潜在的组合生物标志物可以应用于肝细胞癌的早期诊断,并突出了肿瘤蛋白质基因组学在鉴定蛋白质标志物方面的应用,这些蛋白质标志物可以应用于疾病导向的转化医学。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Onco-proteogenomics identifies urinary S100A9 and GRN as potential combinatorial biomarkers for early diagnosis of hepatocellular carcinoma

Hepatocellular carcinoma (HCC), the major type of liver cancer, is among the most lethal cancers owing to its aggressive nature and frequently late detection. Therefore, the possibility to identify early diagnostic markers could be of significant benefit. Urine has especially become one of the most attractive body fluids in biomarker discovery as it can be obtained non-invasively in large quantities and is stable as compared with other body fluids. To identify potential protein biomarker for early diagnosis of HCC, we explored protein expression profiles in urine from HCC patients and normal controls (n = 44) by shotgun proteomics using nano-liquid chromatography coupled tandem mass spectrometry (nanoLC–MS/MS) and stable isotope dimethyl labeling. We have systematically mapped 91 proteins with differential expressions (p < 0.05), which included 8 down-regulated microtubule proteins and 83 up-regulated proteins involved in signal and inflammation response. Further integrated proteogenomic approach composed of proteomic, genomic and transcriptomic analysis identified that S100A9 and GRN were co-amplified (p < 0.001) and co-expressed (p < 0.01) in HCC tumors and urine samples. In addition, the amplifications of S100A9 or GRN were found to be associated with poor survival in HCC patients, and their co-amplification was also prognosed worse overall survival than individual ones. Our results suggest that urinary S100A9 and GRN as potential combinatorial biomarkers can be applied to early diagnosis of hepatocellular carcinoma and highlight the utility of onco-proteogenomics for identifying protein markers that can be applied to disease-oriented translational medicine.

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