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基于通路的胶质母细胞瘤分类揭示了一种具有治疗易感性的线粒体亚型。

Pathway-based classification of glioblastoma uncovers a mitochondrial subtype with therapeutic vulnerabilities.

作者信息

Garofano Luciano, Migliozzi Simona, Oh Young Taek, D'Angelo Fulvio, Najac Ryan D, Ko Aram, Frangaj Brulinda, Caruso Francesca Pia, Yu Kai, Yuan Jinzhou, Zhao Wenting, Di Stefano Anna Luisa, Bielle Franck, Jiang Tao, Sims Peter, Suvà Mario L, Tang Fuchou, Su Xiao-Dong, Ceccarelli Michele, Sanson Marc, Lasorella Anna, Iavarone Antonio

机构信息

Institute for Cancer Genetics, Columbia University Medical Center, New York, NY, USA.

Department of Electrical Engineering and Information Technology, University of Naples Federico II, Naples, Italy.

出版信息

Nat Cancer. 2021 Feb;2(2):141-156. doi: 10.1038/s43018-020-00159-4. Epub 2021 Jan 11.

Abstract

The transcriptomic classification of glioblastoma (GBM) has failed to predict survival and therapeutic vulnerabilities. A computational approach for unbiased identification of core biological traits of single cells and bulk tumors uncovered four tumor cell states and GBM subtypes distributed along neurodevelopmental and metabolic axes, classified as proliferative/progenitor, neuronal, mitochondrial and glycolytic/plurimetabolic. Each subtype was enriched with biologically coherent multiomic features. Mitochondrial GBM was associated with the most favorable clinical outcome. It relied exclusively on oxidative phosphorylation for energy production, whereas the glycolytic/plurimetabolic subtype was sustained by aerobic glycolysis and amino acid and lipid metabolism. Deletion of the glucose-proton symporter was the truncal alteration most significantly associated with mitochondrial GBM, and the reintroduction of SLC45A1 in mitochondrial glioma cells induced acidification and loss of fitness. Mitochondrial, but not glycolytic/plurimetabolic, GBM exhibited marked vulnerability to inhibitors of oxidative phosphorylation. The pathway-based classification of GBM informs survival and enables precision targeting of cancer metabolism.

摘要

胶质母细胞瘤(GBM)的转录组分类未能预测生存率和治疗易损性。一种用于无偏识别单细胞和实体肿瘤核心生物学特征的计算方法揭示了四种肿瘤细胞状态和GBM亚型,它们沿神经发育和代谢轴分布,分类为增殖/祖细胞型、神经元型、线粒体型和糖酵解/多代谢型。每个亚型都富含生物学上连贯的多组学特征。线粒体GBM与最有利的临床结果相关。它完全依赖氧化磷酸化产生能量,而糖酵解/多代谢亚型则由有氧糖酵解以及氨基酸和脂质代谢维持。葡萄糖-质子同向转运体的缺失是与线粒体GBM最显著相关的主干改变,并且在线粒体胶质瘤细胞中重新引入SLC45A1会诱导酸化和适应性丧失。线粒体GBM对氧化磷酸化抑制剂表现出明显的易损性,而糖酵解/多代谢型GBM则不然。基于通路的GBM分类为生存率提供了信息,并能够精准靶向癌症代谢。

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