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首页> 外文期刊>OMICS: A journal of integrative biology >Urine Metabolomic Analysis Identifies Potential Biomarkers and Pathogenic Pathways in Kidney Cancer
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Urine Metabolomic Analysis Identifies Potential Biomarkers and Pathogenic Pathways in Kidney Cancer

机译:尿液代谢组学分析确定潜力生物标志物在肾脏和致病通路癌症

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摘要

Kidney cancer is the seventh most common cancer in the Western world, its incidence is increasing, and it is frequently metastatic at presentation, at which stage patient survival statistics are grim. In addition, there are no useful biofluid markers for this disease, such that diagnosis is dependent on imaging techniques that are not generally used for screening. In the present study, we use metabolomics techniques to identify metabolites in kidney cancer patients' urine, which appear at different levels (when normalized to account for urine volume and concentration) from the same metabolites in nonkidney cancer patients. We found that quinolinate, 4-hydroxybenzoate, and gentisate are differentially expressed at a false discovery rate of 0.26, and these metabolites are involved in common pathways of specific amino acid and energetic metabolism, consistent with high tumor protein breakdown and utilization, and the Warburg effect. When added to four different (three kidney cancer-derived and one "normal") cell lines, several of the significantly altered metabolites, quinolinate, α-ketoglutarate, and gentisate, showed increased or unchanged cell proliferation that was cell line-dependent. Further evaluation of the global metabolomics analysis, as well as confirmation of the specific potential biomarkers using a larger sample size, will lead to new avenues of kidney cancer diagnosis and therapy.
机译:肾癌是第七个最常见的癌症西方世界,其发病率增加,并经常转移在演讲中,在这阶段病人生存的统计数据严峻。标记为这种疾病,诊断不依赖于成像技术一般用于筛查。研究中,我们使用代谢组学技术来识别肾癌患者的尿液中代谢物,时出现在不同的水平(标准化占尿液体积和浓度)从相同的代谢物nonkidney癌症病人。4-hydroxybenzoate,龙胆酸盐错误发现差异表达率0.26,这些代谢物在特定的氨基酸和的共同通路能量代谢,符合高肿瘤和蛋白质分解和利用Warburg效应。(三个肾脏cancer-derived和一个“正常的”)细胞系,几个显著的改变代谢物、quinolinateα酮戊二酸龙胆酸盐,增加或改变细胞细胞line-dependent扩散。进一步评估全球代谢组学分析以及具体的确认使用更大的样本量,潜在的生物标记物将导致肾癌的新途径诊断和治疗。

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