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Functionally distinct subsets of human FOXP3+ Treg cells that phenotypically mirror effector Th cells
被引:324
作者:

Duhen, Thomas
论文数: 0 引用数: 0
h-index: 0
机构:
Benaroya Res Inst, Seattle, WA 98101 USA Benaroya Res Inst, Seattle, WA 98101 USA

Duhen, Rebekka
论文数: 0 引用数: 0
h-index: 0
机构:
Benaroya Res Inst, Seattle, WA 98101 USA Benaroya Res Inst, Seattle, WA 98101 USA

Lanzavecchia, Antonio
论文数: 0 引用数: 0
h-index: 0
机构:
Biomed Res Inst, Bellinzona, Switzerland Benaroya Res Inst, Seattle, WA 98101 USA

Sallusto, Federica
论文数: 0 引用数: 0
h-index: 0
机构:
Biomed Res Inst, Bellinzona, Switzerland Benaroya Res Inst, Seattle, WA 98101 USA

Campbell, Daniel J.
论文数: 0 引用数: 0
h-index: 0
机构:
Benaroya Res Inst, Seattle, WA 98101 USA
Univ Washington, Sch Med, Dept Immunol, Seattle, WA USA Benaroya Res Inst, Seattle, WA 98101 USA
机构:
[1] Benaroya Res Inst, Seattle, WA 98101 USA
[2] Biomed Res Inst, Bellinzona, Switzerland
[3] Univ Washington, Sch Med, Dept Immunol, Seattle, WA USA
来源:
基金:
美国国家卫生研究院;
关键词:
ROR-GAMMA-T;
CHEMOKINE RECEPTOR EXPRESSION;
INTESTINAL INFLAMMATION;
INTERLEUKIN;
22;
T-H-17;
CELLS;
TARGET GENES;
DIFFERENTIATION;
IDENTIFICATION;
CCR6;
TRAFFICKING;
D O I:
10.1182/blood-2011-11-392324
中图分类号:
R5 [内科学];
学科分类号:
1002 ;
100201 ;
摘要:
FOXP3(+) regulatory T (Treg) cells are a broadly acting and potent anti-inflammatory population of CD4(+) T cells essential for maintaining immune homeostasis and preventing debilitating autoimmunity. Based on chemokine receptor expression, we identified distinct populations of Treg cells in human blood expected to colocalize with different Th cell subsets. Although each population was functionally suppressive, they displayed unique patterns of pro- and anti-inflammatory cytokine production, differentially expressed lineage-specifying transcription factors, and responded differently to antigens associated with Th1 and Th17 responses. These results highlight a previously unappreciated degree of phenotypic and functional diversity in human Treg cells that allows subsets with unique specificities and immunomodulatory functions to be targeted to defined immune environments during different types of inflammatory responses. (Blood. 2012;119(19):4430-4440)
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收藏
页码:4430 / 4440
页数:11
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