人类胶质母细胞瘤和患者血浆的代谢组学特征:一项试点研究。

Q2 Pharmacology, Toxicology and Pharmaceutics
F1000Research Pub Date : 2024-09-19 eCollection Date: 2024-01-01 DOI:10.12688/f1000research.143642.3
Yin Allison Liu, Orwa Aboud, Lina A Dahabiyeh, Orin Bloch, Oliver Fiehn
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引用次数: 0

摘要

背景:胶质母细胞瘤(GBM)是一种具有临床挑战性的原发性脑肿瘤,尽管进行了手术切除和强化化疗,但患者的生存率很低。GBM 的代谢异质性可成为治疗反应、耐药性和预后预测的生物标志物。该研究旨在调查原发性和复发性 GBM 组织与患者血浆之间的代谢差异,以确定代谢分析的可行性:一项单中心队列研究使用非靶向代谢组学/脂质组学检测方法分析了15名GBM患者的组织和血液样本。采用非靶向质谱法对诊断和复发时的 GBM 组织和患者血浆进行了代谢组学、脂质组学和生物胺分析。该研究利用一个小型但纵向收集的队列来评估诊断和复发时标本之间代谢物、脂质和生物胺的变化:结果:探索性分析显示,肿瘤和血浆标本中的代谢物、脂类和生物胺在诊断和复发状态之间有明显变化。复发时显著不同的代谢物包括组织中的N-α-甲基组胺、甘油-3-磷酸、磷酸胆碱和琥珀酸,以及血浆中的吲哚-3-乙酸酯和尿素。主成分分析揭示了肿瘤组织和患者血浆之间不同的代谢组学特征。在复发时,GBM 组织和患者血浆中观察到了不同的代谢特征,这证明了使用代谢组学方法进行纵向研究的可行性。一名患者在确诊时表现出独特的肿瘤耐药性特征,可能表明其具有高风险代谢组学表型:在这一小型队列中,研究结果表明,GBM 组织和患者血浆的代谢组学特征具有进行风险分层、结果预测和开发新型代谢靶向辅助疗法的潜力。研究结果表明,组织和血浆在诊断和复发时存在代谢差异,这凸显了对临床反应评估的潜在影响。代谢物丰度的重大变化强调了利用靶向代谢组学进行更大规模研究的必要性,以验证和进一步探索这些特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Metabolomic characterization of human glioblastomas and patient plasma: a pilot study.

Background: Glioblastoma (GBM) is a clinically challenging primary brain tumor with poor survival outcome despite surgical resection and intensive chemoradiation. The metabolic heterogeneity of GBM can become biomarkers for treatment response, resistance, and outcome prediction. The aim of the study is to investigate metabolic distinctions between primary and recurrent GBM tissue and patient plasma to establish feasibility for metabolic profiling.

Methods: A single-center cohort study analyzed tissue and blood samples from 15 patients with GBM using untargeted metabolomic/lipidomic assays. Metabolomic, lipidomic, and biogenic amine analyses were conducted on GBM tissue and patient plasma at diagnosis and recurrence using untargeted mass spectrometry. The study utilized a small but longitudinally collected cohort to evaluate alteration in metabolites, lipids, and biogenic amines between specimens at diagnosis and recurrence.

Results: Exploratory analysis revealed significant alteration in metabolites, lipids, and biogenic amines between diagnostic and recurrent states in both tumor and plasma specimens. Notable metabolites differed at recurrence, including N-alpha-methylhistamine, glycerol-3-phosphate, phosphocholine, and succinic acid in tissue, and indole-3-acetate, and urea in plasma. Principal component analysis revealed distinct metabolomic profiles between tumor tissue and patient plasma. Distinct metabolic profiles were observed in GBM tissue and patient plasma at recurrence, demonstrating the feasibility of using metabolomic methodologies for longitudinal studies. One patient exhibited a unique tumor resistance signature at diagnosis, possibly indicating a high-risk metabolomic phenotype.

Conclusions: In this small cohort, the findings suggest the potential of metabolomic signatures of GBM tissue and patient plasma for risk stratification, outcome prediction, and the development of novel adjuvant metabolic-targeting therapies. The findings suggest metabolic discrepancies at diagnosis and recurrence in tissue and plasma, highlighting potential implications for evaluation of clinical response. The identification of significant changes in metabolite abundance emphasizes the need for larger studies using targeted metabolomics to validate and further explore these profiles.

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来源期刊
F1000Research
F1000Research Pharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (all)
CiteScore
5.00
自引率
0.00%
发文量
1646
审稿时长
1 weeks
期刊介绍: F1000Research publishes articles and other research outputs reporting basic scientific, scholarly, translational and clinical research across the physical and life sciences, engineering, medicine, social sciences and humanities. F1000Research is a scholarly publication platform set up for the scientific, scholarly and medical research community; each article has at least one author who is a qualified researcher, scholar or clinician actively working in their speciality and who has made a key contribution to the article. Articles must be original (not duplications). All research is suitable irrespective of the perceived level of interest or novelty; we welcome confirmatory and negative results, as well as null studies. F1000Research publishes different type of research, including clinical trials, systematic reviews, software tools, method articles, and many others. Reviews and Opinion articles providing a balanced and comprehensive overview of the latest discoveries in a particular field, or presenting a personal perspective on recent developments, are also welcome. See the full list of article types we accept for more information.
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