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Characterization of the serum metabolome following radiation treatment in patients with high-grade gliomas

机译:高级胶质瘤患者放射治疗后血清代谢物的表征

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Background Glioblastomas progress rapidly making response evaluation using MRI insufficient since treatment effects are not detectable until months after initiation of treatment. Thus, there is a strong need for supplementary biomarkers that could provide reliable and early assessment of treatment efficacy. Analysis of alterations in the metabolome may be a source for identification of new biomarker patterns harboring predictive information. Ideally, the biomarkers should be found within an easily accessible compartment such as the blood. Method Using gas-chromatographic- time-of-flight-mass spectroscopy we have analyzed serum samples from 11 patients with glioblastoma during the initial phase of radiotherapy. Fasting serum samples were collected at admittance, on the same day as, but before first treatment and in the morning after the second and fifth dose of radiation. The acquired data was analyzed and evaluated by chemometrics based bioinformatics methods. Our findings were compared and discussed in relation to previous data from microdialysis in tumor tissue, i.e. the extracellular compartment, from the same patients. Results We found a significant change in metabolite pattern in serum comparing samples taken before radiotherapy to samples taken during early radiotherapy. In all, 68 metabolites were lowered in concentration following treatment while 16 metabolites were elevated in concentration. All detected and identified amino acids and fatty acids together with myo-inositol, creatinine, and urea were among the metabolites that decreased in concentration during treatment, while citric acid was among the metabolites that increased in concentration. Furthermore, when comparing results from the serum analysis with findings in tumor extracellular fluid we found a common change in metabolite patterns in both compartments on an individual patient level. On an individual metabolite level similar changes in ornithine, tyrosine and urea were detected. However, in serum, glutamine and glutamate were lowered after treatment while being elevated in the tumor extracellular fluid. Conclusion Cross-validated multivariate statistical models verified that the serum metabolome was significantly changed in relation to radiation in a similar pattern to earlier findings in tumor tissue. However, all individual changes in tissue did not translate into changes in serum. Our study indicates that serum metabolomics could be of value to investigate as a potential marker for assessing early response to radiotherapy in malignant glioma.
机译:背景技术胶质母细胞瘤开始使用MRI快速进行响应评估,因为在治疗开始后的几个月后治疗效果是不可检测的。因此,对辅助生物标志物有很强的需求,可以提供对治疗效果的可靠和早期评估。分析代谢物中的改变可能是鉴定涉及预测信息的新生物标志物模式的源。理想情况下,生物标志物应在易于达到血液的易于可访问的隔间内找到。使用气相色谱 - 飞行时间质谱的方法,我们在放疗初始阶段分析了11例胶质母细胞瘤患者的血清样本。在当天的情况下收集禁食血清样品,但在第一次治疗之前,在第二和第五剂辐射后的早晨,在早晨。通过基于化学计量学的生物信息学方法分析和评估所获得的数据。比较了我们的研究结果,并与来自肿瘤组织中的微透析中的先前数据相关,即来自同一患者的细胞外隔室。结果我们发现血清中代谢物模式的显着变化比较在放疗前取代的样品到早期放射治疗期间采样的样品。在所有情况下,在治疗后浓度降低了68种代谢物,而16代谢物浓度升高。所有检测和鉴定的氨基酸和脂肪酸与肌肌醇,肌酐和尿素一起含有浓度在治疗期间减少的代谢产物中,而柠檬酸是浓度增加的代谢物中。此外,当与肿瘤细胞外液中的结果进行血清分析的结果进行比较时,我们发现在个体患者水平上的两个隔间中的代谢物模式的常见变化。在单个代谢物水平上,鸟氨酸的相似变化,检测酪氨酸和尿素。然而,在血清中,处理后谷氨酰胺和谷氨酸在肿瘤细胞外液中升高时降低。结论交叉验证多元统计模型证实,与肿瘤组织中的早期发现的类似模式的辐射有关血清代谢物显着改变。然而,组织的所有个体变化都没有转化为血清的变化。我们的研究表明,血清代谢组学可能具有值,以调查作为评估恶性胶质瘤中放射治疗的早期反应的潜在标志物。

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