Proteomic Analyses of Human Regulatory T Cells Reveal Adaptations in Signaling Pathways that Protect Cellular Identity

被引:103
作者
Cuadrado, Eloy [1 ]
van den Biggelaar, Maartje [2 ]
de Kivit, Sander [3 ]
Chen, Yi-yen [3 ]
Slot, Manon [1 ]
Doubal, Ihsane [1 ]
Meijer, Alexander [2 ]
van Lier, Rene A. W. [1 ]
Borst, Jannie [3 ]
Amsen, Derk [1 ]
机构
[1] Univ Amsterdam, Acad Med Ctr, Dept Hematopoiesis, Sanquin Res & Landsteiner Lab, Amsterdam, Netherlands
[2] Univ Amsterdam, Acad Med Ctr, Dept Plasma Prot, Sanquin Res & Landsteiner Lab, Amsterdam, Netherlands
[3] Netherlands Canc Inst Antoni van Leeuwenhoek, Div Tumor Biol & Immunol, NL-1066 CX Amsterdam, Netherlands
关键词
TRANSCRIPTION FACTOR FOXP3; NF-KAPPA-B; SUPPRESSIVE ACTIVITY; NEGATIVE REGULATOR; GENE-EXPRESSION; IN-VIVO; DIFFERENTIATION; INFLAMMATION; ACTIVATION; COMPLEX;
D O I
10.1016/j.immuni.2018.04.008
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
To obtain a molecular definition of regulatory T (Treg) cell identity, we performed proteomics and transcriptomics on various populations of human regulatory and conventional CD4(+) T (Tconv) cells. A protein expression signature was identified that defines all Treg cells, and another signature that defines effector Treg cells. These signatures could not be extrapolated from transcriptome data. Unique cellbiological and metabolic features in Treg cells were defined, as well as specific adaptations in cytokine, TCR, and costimulatory receptor signaling pathways. One such adaptation-selective STAT4 deficiency-prevented destabilization of Treg cell identity and function by inflammatory cytokines, while these signals could still induce critical transcription factors and homing receptors via other pathways. Furthermore, our study revealed surface markers that identify FOXP3(+)CD4(+) T cells with distinct functional properties. Our findings suggest that adaptation in signaling pathways protect Treg cell identity and present a resource for further research into Treg cell biology.
引用
收藏
页码:1046 / +
页数:20
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