Thymic regulatory T cells arise via two distinct developmental programs

被引:155
|
作者
Owen, David L. [1 ,2 ]
Mahmud, Shawn A. [1 ,2 ]
Sjaastad, Louisa E. [1 ,2 ]
Williams, Jason B. [3 ]
Spanier, Justin A. [4 ]
Simeonov, Dimitre R. [5 ,6 ,7 ]
Ruscher, Roland [1 ,2 ]
Huang, Weishan [8 ,9 ]
Proekt, Irina [6 ]
Miller, Corey N. [6 ]
Hekim, Can [1 ,2 ]
Jeschke, Jonathan C. [3 ]
Aggarwal, Praful [10 ]
Broeckel, Ulrich [10 ]
LaRue, Rebecca S. [11 ]
Henzler, Christine M. [11 ]
Alegre, Maria-Luisa [12 ]
Anderson, Mark S. [6 ,13 ]
August, Avery [8 ]
Marson, Alexander [5 ,6 ,13 ,14 ,15 ]
Zheng, Ye [16 ]
Williams, Calvin B. [3 ]
Farrar, Michael A. [1 ,2 ]
机构
[1] Univ Minnesota, Ctr Immunol, Masonic Canc Ctr, Minneapolis, MN 55455 USA
[2] Univ Minnesota, Dept Lab Med & Pathol, Minneapolis, MN 55455 USA
[3] Med Coll Wisconsin, Dept Pediat, Sect Rheumatol, 8701 Watertown Plank Rd, Milwaukee, WI 53226 USA
[4] Univ Minnesota, Dept Med, Ctr Immunol, Box 736 UMHC, Minneapolis, MN 55455 USA
[5] Univ Calif San Francisco, Dept Microbiol & Immunol, San Francisco, CA 94143 USA
[6] Univ Calif San Francisco, Diabet Ctr, San Francisco, CA 94143 USA
[7] Univ Calif San Francisco, Biomed Sci Grad Program, San Francisco, CA 94143 USA
[8] Cornell Univ, Coll Vet Med, Dept Microbiol & Immunol, Ithaca, NY 14853 USA
[9] Louisiana State Univ, Sch Vet Med, Dept Pathobiol Sci, Baton Rouge, LA 70803 USA
[10] Med Coll Wisconsin, Dept Pediat, Sect Genom Pediat, 8701 Watertown Plank Rd, Milwaukee, WI 53226 USA
[11] Univ Minnesota, Supercomputing Inst Adv Computat Res, Minneapolis, MN USA
[12] Univ Chicago, Dept Med, Sect Rheumatol, 5841 S Maryland Ave, Chicago, IL 60637 USA
[13] Univ Calif San Francisco, Dept Med, San Francisco, CA USA
[14] Chan Zuckerberg Biohub, San Francisco, CA USA
[15] Univ Calif Berkeley, Innovat Genom Inst, Berkeley, CA 94720 USA
[16] Salk Inst Biol Studies, Nomis Fdn Labs Immunobiol & Microbial Pathogenesi, 10010 N Torrey Pines Rd, La Jolla, CA 92037 USA
来源
NATURE IMMUNOLOGY | 2019年 / 20卷 / 02期
基金
美国国家卫生研究院;
关键词
FOXP3 TRANSCRIPTION FACTOR; NF-KAPPA-B; COSTIMULATORY REQUIREMENTS; THYMOCYTE DEVELOPMENT; SIGNAL STRENGTH; SELF-PEPTIDES; RECEPTOR; TOLERANCE; GENE; TCR;
D O I
10.1038/s41590-018-0289-6
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The developmental programs that generate a broad repertoire of regulatory T cells (T-reg cells) able to respond to both self antigens and non-self antigens remain unclear. Here we found that mature T-reg cells were generated through two distinct developmental programs involving CD25(+) T-reg cell progenitors (CD25(+) TregP cells) and Foxp3(lo) T-reg cell progenitors (Foxp3(lo) TregP cells). CD25(+) TregP cells showed higher rates of apoptosis and interacted with thymic self antigens with higher affinity than did Foxp3(lo) TregP cells, and had a T cell antigen receptor repertoire and transcriptome distinct from that of Foxp3(lo) TregP cells. The development of both CD25(+) TregP cells and Foxp3(lo) TregP cells was controlled by distinct signaling pathways and enhancers. Transcriptomics and histocytometric data suggested that CD25(+) TregP cells and Foxp3(lo) TregP cells arose by coopting negative-selection programs and positive-selection programs, respectively. T-reg cells derived from CD25(+) TregP cells, but not those derived from Foxp3(lo) TregP cells, prevented experimental autoimmune encephalitis. Our findings indicate that T-reg cells arise through two distinct developmental programs that are both required for a comprehensive T-reg cell repertoire capable of establishing immunotolerance.
引用
收藏
页码:195 / +
页数:17
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