Glutamine blockade induces divergent metabolic programs to overcome tumor immune evasion

被引:773
|
作者
Leone, Robert D. [1 ]
Zhao, Liang [1 ]
Englert, Judson M. [1 ]
Sun, Im-Meng [1 ]
Oh, Min-Hee [1 ]
Sun, Im-Hong [1 ]
Arwood, Matthew L. [1 ]
Bettencourt, Ian A. [1 ]
Patel, Chirag H. [1 ]
Wen, Jiayu [1 ]
Tam, Ada [1 ]
Blosser, Richard L. [1 ]
Prchalova, Eva [2 ]
Alt, Jesse [2 ]
Rais, Rana [2 ]
Slusher, Barbara S. [2 ]
Powell, Jonathan D. [1 ]
机构
[1] Johns Hopkins, Bloomberg Kimmel Inst Canc Immunotherapy, Baltimore, MD 21287 USA
[2] Johns Hopkins Sch Med, Johns Hopkins Drug Discovery, Baltimore, MD 21205 USA
来源
SCIENCE | 2019年 / 366卷 / 6468期
基金
美国国家卫生研究院;
关键词
PYRUVATE-CARBOXYLASE; PHASE-II; 6-DIAZO-5-OXO-L-NORLEUCINE DON; T-CELLS; CANCER; MYC; INHIBITION; REGULATOR; DELIVERY; PRODRUG;
D O I
10.1126/science.aav2588
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
The metabolic characteristics of tumors present considerable hurdles to immune cell function and cancer immunotherapy. Using a glutamine antagonist, we metabolically dismantled the immunosuppressive microenvironment of tumors. We demonstrate that glutamine blockade in tumor-bearing mice suppresses oxidative and glycolytic metabolism of cancer cells, leading to decreased hypoxia, acidosis, and nutrient depletion. By contrast, effector T cells responded to glutamine antagonism by markedly up-regulating oxidative metabolism and adopting a long-lived, highly activated phenotype. These divergent changes in cellular metabolism and programming form the basis for potent antitumor responses. Glutamine antagonism therefore exposes a previously undefined difference in metabolic plasticity between cancer cells and effector T cells that can be exploited as a "metabolic checkpoint" for tumor immunotherapy.
引用
收藏
页码:1013 / +
页数:41
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