首页> 外文期刊>Cancer: A Journal of the American Cancer Society >Large‐scale profiling of serum metabolites in African American and European American patients with bladder cancer reveals metabolic pathways associated with patient survival
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Large‐scale profiling of serum metabolites in African American and European American patients with bladder cancer reveals metabolic pathways associated with patient survival

机译:非洲裔美国和欧洲膀胱癌患者血清代谢物的大规模谱分析显示出与患者生存相关的代谢途径

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Background African Americans (AAs) experience a disproportionally high rate of bladder cancer (BLCA) deaths even though their incidence rates are lower than those of other patient groups. Using a metabolomics approach, this study investigated how AA BLCA may differ molecularly from European Americans (EAs) BLCA, and it examined serum samples from patients with BLCA with the aim of identifying druggable metabolic pathways in AA patients. Methods Targeted metabolomics was applied to measure more than 300 metabolites in serum samples from 2 independent cohorts of EA and AA patients with BLCA and healthy EA and AA controls via liquid chromatography–mass spectrometry, and this was followed by the identification of altered metabolic pathways with a focus on AA BLCA. A subset of the differential metabolites was validated via absolute quantification with the Biocrates AbsoluteIDQ p180 kit. The clinical significance of the findings was further examined in The Cancer Genomic Atlas BLCA data set. Results Fifty‐three metabolites, mainly related to amino acid, lipid, and nucleotide metabolism, were identified that showed significant differences in abundance between AA and EA BLCA. For example, the levels of taurine, glutamine, glutamate, aspartate, and serine were elevated in serum samples from AA patients versus EA patients. By mapping these metabolites to genes, this study identified significant relations with regulators of metabolism such as malic enzyme 3, prolyl 3‐hydroxylase 2, and lysine demethylase 2A that predicted patient survival exclusively in AA patients with BLCA. Conclusions This metabolic profile of serum samples might be used to assess risk progression in AA BLCA. These first‐in‐field findings describe metabolic alterations in AA BLCA and emphasize a potential biological basis for BLCA health disparities.
机译:背景技术即使它们的发病率低于其他患者群体,也会经历不成比例的膀胱癌(BLCA)死亡率。使用代谢组种方法,本研究研究了AA BLCA如何与欧洲美国人(EAS)BLCA不同的分子,并且它检查了BLCA患者的血清样本,目的是鉴定AA患者的可药剂代谢途径。方法采用靶向代谢物测量来自2株血清样品的血清样品中的300多个代谢物,并通过液相色谱 - 质谱法测量来自BLCA和健康EA和AA对照的AA对照的血清样品中,然后鉴定改变的代谢途径专注于AA Blca。通过用BIOCRATESIOMIDQ P180套件通过绝对量化验证差分代谢物的子集。在癌症基因组地图集BLCA数据集中进一步检查了结果的临床意义。结果鉴定了五十三种代谢物,主要与氨基酸,脂质和核苷酸代谢相关,鉴定出AA和EA BLCA之间的丰富差异显着差异。例如,牛磺酸,谷氨酰胺,谷氨酸,天冬氨酸和丝氨酸的水平在来自AA患者的血清样品中升高了EA患者。通过将这些代谢产物映射到基因,本研究确定了与代谢调节剂的显着关系,例如苹果酶3,脯氨酰3-羟化酶2和赖氨酸脱甲基化酶2a,其在AA患者中预测患者存活率。结论血清样品的这种代谢型材可用于评估AA BLCA的风险进展。这些先前发现描述了AA BLCA的代谢改变,并强调了BLCA卫生差异的潜在生物学基础。

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