通过c-MET抑制代谢重编程作为胶质母细胞瘤的可靶向脆弱性。

Oncoscience Pub Date : 2020-03-20 eCollection Date: 2020-01-01 DOI:10.18632/oncoscience.498
Trang Thi Thu Nguyen, Enyuan Shang, Georg Karpel-Massler, Markus D Siegelin
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引用次数: 2

摘要

阐明更好的治疗实体瘤,特别是恶性胶质瘤是当务之急。更好地了解治疗反应和耐药性的分子基础是这一努力成功的关键决定因素。最近,一系列新的工具浮出水面,这些工具可以比早期更精确地询问肿瘤细胞代谢。这些发展的前沿是细胞外通量和碳追踪分析。通过利用这些技术,我们的团队最近观察到急性和慢性c-MET抑制会驱动脂肪酸氧化,从而可以作为药物联合治疗的治疗目标。在此,我们对与本研究相关的一些关键发现进行总结和评论。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Metabolic Reprogramming by c-MET Inhibition as a Targetable Vulnerability in Glioblastoma.

The elucidation of better treatments for solid tumors and especially malignant glial tumors is a priority. Better understanding of the molecular underpinnings of treatment response and resistance are critical determinants in the success for this endeavor. Recently, a battery of novel tools have surfaced that allow to interrogate tumor cell metabolism to more precise extent than this was possible in the earlier days. At the forefront of these developments are the extracellular flux and carbon tracing analyses. Through utilization of these techniques our group made the recent observation that acute and chronic c-MET inhibition drives fatty acid oxidation that in turn can be therapeutically targeted for drug combination therapies. Herein, we summarize and comment on some of our key findings related to this study.

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