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GITR Intrinsically Sustains Early Type 1 and Late Follicular Helper CD4 T Cell Accumulation to Control a Chronic Viral Infection

机译：GITR本质上维持早期1型和晚期卵泡辅助CD4 T细胞的积累以控制慢性病毒感染。

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CD4 T cells are critical for control of persistent infections; however, the key signals that regulate CD4 T help during chronic infection remain incompletely defined. While several studies have addressed the role of inhibitory receptors and soluble factors such as PD-1 and IL-10, significantly less work has addressed the role of T cell co-stimulatory molecules during chronic viral infection. Here we show that during a persistent infection with lymphocytic choriomeningitis virus (LCMV) clone 13, mice lacking the glucocorticoid-induced tumor necrosis factor receptor related protein (GITR) exhibit defective CD8 T cell accumulation, increased T cell exhaustion and impaired viral control. Differences in CD8 T cells and viral control between GITR^+/+ and GITR^-/- mice were lost when CD4 T cells were depleted. Moreover, mixed bone marrow chimeric mice, as well as transfer of LCMV epitope-specific CD4 or CD8 T cells, demonstrated that these effects of GITR are largely CD4 T cell-intrinsic. GITR is dispensable for initial CD4 T cell proliferation and differentiation, but supports the post-priming accumulation of IFNγ⁺IL-2⁺ Th1 cells, facilitating CD8 T cell expansion and early viral control. GITR-dependent phosphorylation of the p65 subunit of NF-κB as well as phosphorylation of the downstream mTORC1 target, S6 ribosomal protein, were detected at day three post-infection (p.i.), and defects in CD4 T cell accumulation in GITR-deficient T cells were apparent starting at day five p.i. Consistently, we pinpoint IL-2-dependent CD4 T cell help for CD8 T cells to between days four and eight p.i. GITR also increases the ratio of T follicular helper to T follicular regulatory cells and thereby enhances LCMV-specific IgG production. Together, these findings identify a CD4 T cell-intrinsic role for GITR in sustaining early CD8 and late humoral responses to collectively promote control of chronic LCMV clone 13 infection.

机译：CD4 T细胞对于控制持续感染至关重要。但是，在慢性感染期间调节CD4 T帮助的关键信号仍未完全确定。尽管一些研究已经解决了抑制性受体和可溶性因子（例如PD-1和IL-10）的作用，但是，在慢性病毒感染过程中，T细胞共刺激分子的作用却大大减少了。在这里，我们显示在持续感染淋巴细胞性脉络膜脑膜炎病毒（LCMV）克隆13期间，缺少糖皮质激素诱导的肿瘤坏死因子受体相关蛋白（GITR）的小鼠表现出缺陷的CD8 T细胞蓄积，T细胞衰竭和病毒控制受损。耗尽CD4 T细胞后，GITR ^{+ / + 和GITR ^{-/-小鼠之间CD8 T细胞和病毒控制的差异消失了。此外，混合的骨髓嵌合体小鼠以及LCMV表位特异性CD4或CD8 T细胞的转移证明，GITR的这些作用很大程度上是CD4 T细胞固有的。 GITR对于CD4 T细胞的初始增殖和分化是必不可少的，但它支持IFNγ^{+ IL-2 ^{+ Th1细胞的引发后积累，从而促进CD8 T细胞的扩增和早期病毒控制。在感染后第3天（pi）检测到GITR依赖的NF-κBp65亚基的GITR磷酸化，以及下游mTORC1靶标S6核糖体蛋白的磷酸化，以及GITR缺陷型T中CD4 T细胞积累的缺陷在感染后第5天开始出现细胞一致地，我们将IL-8依赖的CD4 T细胞对CD8 T细胞的帮助精确定位在p.i的第4至8天之间。 GITR还增加了T卵泡辅助细胞与T卵泡调节细胞的比例，从而提高了LCMV特异性IgG的产生。在一起，这些发现确定了GITR在维持早期CD8和晚期体液反应以共同促进慢性LCMV克隆13感染控制中的CD4 T细胞内在作用。}}}}

著录项

期刊名称 PLoS Pathogens
作者
Derek L. Clouthier; Angela C. Zhou; Michael E. Wortzman; Olga Luft; Gary A. Levy; Tania H. Watts;
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作者单位

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年(卷),期 2015(11),1
年度 2015
页码 e1004517
总页数 21
原文格式 PDF
正文语种
中图分类微生物学;寄生动物、寄生虫学;医学寄生虫学;人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. GITR Intrinsically Sustains Early Type 1 and Late Follicular Helper CD4 T Cell Accumulation to Control a Chronic Viral Infection [J] . Derek L. Clouthier, Angela C. Zhou, Michael E. Wortzman, PLoS Pathogens . 2015,第1期

机译：GITR本质上维持早期1型和晚期卵泡辅助CD4 T细胞积累，以控制慢性病毒感染。
2. GITR Intrinsically Sustains Early Type 1 and Late Follicular Helper CD4 T Cell Accumulation to Control a Chronic Viral Infection [J] . Derek L. Clouthier, Angela C. Zhou, Michael E. Wortzman, PLoS Pathogens . 2015,第1期

机译：GITR本质上维持早期1型和晚期卵泡辅助CD4 T细胞积累，以控制慢性病毒感染。
3. Late lnterleukin-6 Escalates T Follicular Helper Cell Responses and Controls a Chronic Viral Infection [J] . James A. Harker, Gavin M. Lewis, Lauren Mack, Science . 2011,第6057期

机译：晚期白介素6升级了T卵泡辅助细胞的反应，并控制了慢性病毒感染。
4. Global Dynamics of a Viral Infection Model with Chronically Infected Cells Response [C] . Shifei Wang, Yicang Zhou International congress on mathematical biology;ICMB2011 . 2011

机译：具有慢性感染细胞反应的病毒感染模型的全局动力学。
5. Dendritic cells and CD4+ T cells: Dual roles in the clearance and pathogenesis of herpes simplex type 1 viral infection . [D] . Frank, Gregory Mettauer. 2010

机译：树突状细胞和CD4 + T细胞：在单纯疱疹1型病毒感染的清除和发病机理中起双重作用。
6. Late Interleukin-6 escalates T follicular helper cell responses and controls a chronic viral infection [O] . James A. Harker, Gavin M. Lewis, Lauren Mack, -1

机译：晚白细胞介素-6升级Ť滤泡辅助细胞应答和控制的慢性病毒感染
7. GITR intrinsically sustains early type 1 and late follicular helper CD4 T cell accumulation to control a chronic viral infection. [O] . Derek L Clouthier, Angela C Zhou, Michael E Wortzman, 2015

机译：GITR本质上维持早期1型和晚期滤泡辅助CD4 T细胞积聚以控制慢性病毒感染。

GITR Intrinsically Sustains Early Type 1 and Late Follicular Helper CD4 T Cell Accumulation to Control a Chronic Viral Infection

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