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Suppression of antitumor T cell immunity by the oncometabolite (R)-2-hydroxyglutarate.

Nat. Med.. 2018; 
BunseLukas,PuschStefan,BunseTheresa,SahmFelix,SanghviKhwab,FriedrichMirco,AlansaryDalia,SonnerJana K,GreenEdward,DeumelandtKatrin,KilianMichael,NeftelCyril,UhligStefanie,KesslerTobias,von LandenbergAnna,BerghoffAnna S,MarshKelly,SteadmanMya,ZhuDongwei,NicolayBrandon,WiestlerBenedikt,BreckwoldtMichael O,Al-AliRuslan,Karcher-BauschSimone,BozzaMatthias,OezenIris,KramerMagdalena,MeyerJochen,HabelAntje,EiselJessica,PoschetGernot,WellerMichael,PreusserMatthias,Nadji-OhlMinou,ThonNiklas,BurgerMichael C,HarterPatrick N,RatliffMiriam,HarbottleRichard,BennerAxel,SchrimpfDaniel,OkunJürgen,Herold-MendeChristel,TurcanSevin,KaulfussStefan,Hess-StumppHolger,BiebackKaren,CahillDaniel P,PlateKarl H,HänggiDaniel,DorschMarion,SuvàMario L,NiemeyerBarbara A,von DeimlingAndreas,WickWolfgang,PlattenMic
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摘要

The oncometabolite (R)-2-hydroxyglutarate (R-2-HG) produced by isocitrate dehydrogenase (IDH) mutations promotes gliomagenesis via DNA and histone methylation. Here, we identify an additional activity of R-2-HG: tumor cell-derived R-2-HG is taken up by T cells where it induces a perturbation of nuclear factor of activated T cells transcriptional activity and polyamine biosynthesis, resulting in suppression of T cell activity. IDH1-mutant gliomas display reduced T cell abundance and altered calcium signaling. Antitumor immunity to experimental syngeneic IDH1-mutant tumors induced by IDH1-specific vaccine or checkpoint inhibition is improved by inhibition of the neomorphic enzymatic function of mutant IDH1. T... More

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