Idd9.1 Locus Controls the Suppressive Activity of FoxP3+CD4+CD25+ Regulatory T-Cells

被引:28
作者
Yamanouchi, Jun [1 ,2 ]
Puertas, Maria-Carmen [3 ,6 ]
Verdaguer, Joan [3 ,6 ]
Lyons, Paul A. [4 ]
Rainbow, Daniel B. [4 ]
Chamberlain, Giselle [4 ]
Hunter, Kara M. [4 ]
Peterson, Laurence B. [5 ]
Wicker, Linda S. [4 ]
Santamaria, Pere [1 ,2 ]
机构
[1] Univ Calgary, Fac Med, Julia McFarlane Diabet Res Ctr, Calgary, AB, Canada
[2] Univ Calgary, Fac Med, Inst Infect Immun & Inflammat, Dept Microbiol & Infect Dis, Calgary, AB, Canada
[3] Univ Lleida, Fac Med, Dept Expt Med, Unitat Immunol, Lleida, Spain
[4] Univ Cambridge, Cambridge Inst Med Res, Dept Med Genet,Diabet & Inflammat Lab, Juvenile Diabet Res Fdn Wellcome Trust, Cambridge, England
[5] Merck Res Labs, Rahway, NJ USA
[6] IRB Lleida, Lleida, Spain
来源
DIABETES | 2010年 / 59卷 / 01期
基金
英国惠康基金; 加拿大健康研究院; 美国国家卫生研究院;
关键词
NONOBESE DIABETIC MICE; LYMPHOID TYROSINE PHOSPHATASE; GENOME-WIDE ASSOCIATION; NOD MICE; AVIDITY MATURATION; CONGENIC MICE; SUSCEPTIBILITY; GENE; REGION; CTLA4;
D O I
10.2337/db09-0648
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
OBJECTIVE-The similar to 45-cM insulin-dependent diabetes 9 (Idd9) region on mouse chromosome 4 harbors several different type I diabetes-associated loci. Nonobese diabetic (NOD) mice congenic for the Idd9 region of C57BL/10 (B10) mice, carrying antidiabetogenic alleles in three different Idd9 subregions (Idd9.1, Idd9.2, and Idd9.3), are strongly resistant to type 1 diabetes. However, the mechanisms remain unclear. This study aimed to define mechanisms underlying the type 1 diabetes resistance afforded by B10 Idd9.1, Idd9.2, and/or Idd9.3. RESEARCH DESIGN AND METHODS-We used a reductionist approach that involves comparing the fate of a type 1 diabetes-relevant autoreactive CD8(+) T-cell population, specific for residues 206-214 of islet-specific glucose 6 phosphatase catalytic subunit-related protein (IGRP(206-214)), in noncongenic versus B10 Idd9-congenic (Idd9.1 + Idd9.2 + Idd9.3, Idd9.2 + Idd9.3, Idd9. 1, Idd9.2, and Idd9. 3) T-cell receptor (TCR)-transgenic (8.3) NOD mice. RESULTS-Most of the protective effect of Idd9 against 8.3-CD8(+) T-cell-enhanced type 1 diabetes was mediated by Idd9.1. Although Idd9.2 and Idd9.3 afforded some protection, the effects were small and did not enhance the greater protective effect of Idd9.1. B10 Idd9.1 afforded type 1 diabetes resistance without impairing the developmental biology or intrinsic diabetogenic potential of autoreactive CD8(+) T-cells. Studies in T- and B-cell-deficient 8.3-NOD.B10 Idd9.1 mice revealed that this antidiabetogenic effect was mediated by endogenous, nontransgenic T-cells in a B-cell-independent manner. Consistent with this, B10 Idd9.1 increased the suppressive function and antidiabetogenic activity of the FoxP3(+)CD4(+)CD25(+) T-cell subset in both TCR-transgenic and nontransgenic mice. CONCLUSIONS-A gene(s) within Idd9.1 regulates the development and function of FoyP3(+)CD4(+)CD25(+) regulatory T-cells and, in turn, the activation of CD8+ effector T-cells in the pancreatic draining lymph nodes, without affecting their development or intrinsic diabetogenic potential. Diabetes 59:272-281,2010
引用
收藏
页码:272 / 281
页数:10
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