Interleukin-17 Accelerates Allograft Rejection by Suppressing Regulatory T Cell Expansion

被引：71

作者：

Itoh, Satoshi ^{[1
]}

Kimura, Naoyuki ^{[1
,3
]}

Axtell, Robert C. ^{[2
]}

Velotta, Jeffrey B. ^{[1
]}

Gong, Yongquan ^{[1
]}

Wang, Xi ^{[1
]}

Kajiwara, Naoki ^{[4
]}

Nambu, Aya ^{[3
]}

Shimura, Eri ^{[3
]}

Adachi, Hideo ^{[7
]}

Iwakura, Yoichiro ^{[6
]}

Saito, Hirohisa ^{[4
]}

Okumura, Ko ^{[3
]}

Sudo, Katsuko ^{[8
]}

Steinman, Lawrence ^{[2
]}

Robbins, Robert C. ^{[1
]}

Nakae, Susumu ^{[5
]}

Fischbein, Michael P. ^{[1
]}

机构：

[1] Stanford Univ, Sch Med, Dept Cardiothorac Surg, Stanford, CA 94305 USA

[2] Stanford Univ, Sch Med, Dept Neurol & Neurol Sci, Stanford, CA 94305 USA

[3] Juntendo Univ, Atopy Res Ctr, Tokyo, Japan

[4] Natl Res Inst Child Hlth & Dev, Dept Allergy & Immunol, Tokyo, Japan

[5] Univ Tokyo, Inst Med Sci, Ctr Expt Med & Syst Biol, Frontier Res Initiat,Lab Syst Biol,Minatu Ku, Tokyo 1088639, Japan

[6] Univ Tokyo, Inst Med Sci, Lab Mol Pathogenesis, Tokyo 1088639, Japan

[7] Jichi Med Univ, Saitama Med Ctr, Dept Cardiovasc Surg, Saitama, Japan

[8] Tokyo Med Univ, Anim Res Ctr, Tokyo, Japan

来源：

CIRCULATION | 2011年 / 124卷 / 11期

关键词：

acute allograft rejection; gamma delta; IL-17; regulatory T cell; T cell; TRANSPLANTATION TOLERANCE; IMMUNE-RESPONSES; GRAFT-REJECTION; TH17; CELLS; GAMMA; IL-17; LUNG; LYMPHOCYTES; NECROSIS; PROMOTES;

D O I：

10.1161/CIRCULATIONAHA.110.014852

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Background-Interleukin-17 (IL-17), which is predominantly produced by T helper 17 cells distinct from T helper 1 or T helper 2 cells, participates in the pathogenesis of infectious, autoimmune, and allergic disorders. However, the precise role in allograft rejection remains uncertain. In the present study, we investigated the role of IL-17 in acute allograft rejection using IL-17-deficient mice. Methods and Results-Donor hearts from FVB mice were heterotopically transplanted into either C57BL/6J-IL-17-deficient (IL-17(-/-)) or -wild-type mice. Allograft survival was significantly prolonged in IL-17(-/-) recipient mice due to reduced local inflammation accompanied by decreased inflammatory cell recruitment and cytokine/chemokine expression. IL-17(-/-) recipient mice exhibited decreased IL-6 production and reciprocally enhanced regulatory T cell expansion, suggesting a contribution of regulatory T cells to prolonged allograft survival. Indeed, allografts transplanted into anti-CD25 mAb-treated IL-17(-/-) recipient mice (regulatory T cell-depleted) developed acute rejection similar to wild-type recipient mice. Surprisingly, we found that gamma delta T cells rather than CD4(+) and CD8(+) T cells were key IL-17 producers in the allografts. In support, equivalent allograft rejection was observed in Rag-2(-/-) recipient mice engrafted with either wild-type or IL-17(-/-) CD4(+) and CD8(+) T cells. Finally, hearts transplanted into gamma delta T cell-deficient mice resulted in decreased allograft rejection compared with wild-type controls. Conclusions-During heart transplantation, (1) IL-17 is crucial for acceleration of acute rejection; (2) IL-17-deficiency enhances regulatory T cell expansion; and (3) gamma delta T cells rather than CD4(+) and CD8(+) T cells are a potential source of IL-17. IL-17 neutralization may provide a potential target for novel therapeutic treatment for cardiac allograft rejection. (Circulation. 2011;124[suppl 1]:S187-S196.)

引用

页码：S187 / S196

页数：10

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