Cutting edge: adaptive versus innate receptor signals selectively control the pool sizes of murine IFN-gamma- or IL-17-producing gammadelta T cells upon infection.

Ribot JC; Chaves Ferreira M; dOrey F; Wencker M; Goncalves Sousa N; Decalf J; Simas JP; Hayday AC; Silva Santos B

首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cutting edge: adaptive versus innate receptor signals selectively control the pool sizes of murine IFN-gamma- or IL-17-producing gammadelta T cells upon infection.

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Cutting edge: adaptive versus innate receptor signals selectively control the pool sizes of murine IFN-gamma- or IL-17-producing gammadelta T cells upon infection.

机译：前沿：适应性信号与先天性受体信号在感染后选择性地控制产生鼠IFN-γ或IL-17的γδT细胞的库大小。

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gammadelta T lymphocytes are commonly viewed as embracing properties of both adaptive and innate immunity. Contributing to this is their responsiveness to pathogen products, either with or without the involvement of the TCR and its coreceptors. This study clarifies this paradoxical behavior by showing that these two modes of responsiveness are the properties of two discrete sets of murine lymphoid gammadelta T cells. Thus, MyD88 deficiency severely impaired the response to malaria infection of CD27((-)), IL-17A-producing gammadelta T cells, but not of IFN-gamma-producing gammadelta cells. Instead, the latter compartment was severely contracted by ablating CD27, which synergizes with TCRgammadelta in the induction of antiapoptotic mediators and cell cycle-promoting genes in CD27((+)), IFN-gamma-secreting gammadelta T cells. Hence, innate versus adaptive receptors differentially control the peripheral pool sizes of discrete proinflammatory gammadelta T cell subsets during immune responses to infection.

机译：γT淋巴细胞通常被视为具有适应性免疫和先天性免疫的特性。造成这种情况的原因是它们对病原体产品的响应能力，无论是否有TCR及其共受体参与。这项研究通过证明这两种反应方式是两组离散的鼠淋巴γ-T细胞的特性，从而澄清了这种自相矛盾的行为。因此，MyD88缺乏严重削弱了对CD27（（-）），IL-17A产生的γ-T细胞对疟疾感染的反应，但对IFN-γ产生的γ细胞却没有造成损害。取而代之的是，后者的腔室被消融的CD27严重收缩，CD27与TCRgammadelta协同诱导CD27（（+）），分泌IFN-γ的γ-δT细胞中的抗凋亡介质和细胞周期促进基因。因此，先天性与适应性受体在对感染的免疫反应过程中差异地控制离散的促炎性γT细胞亚群的外周池大小。

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《The Journal of Immunology: Official Journal of the American Association of Immunologists 》 |2010年第11期| 共5页
作者
Ribot JC; Chaves Ferreira M; dOrey F; Wencker M; Goncalves Sousa N; Decalf J; Simas JP; Hayday AC; Silva Santos B;
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1. Cutting edge: adaptive versus innate receptor signals selectively control the pool sizes of murine IFN-gamma- or IL-17-producing gammadelta T cells upon infection. [J] . Ribot JC, Chaves Ferreira M, dOrey F, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2010 ,第11期

机译：前沿：适应性信号与先天性受体信号在感染后选择性地控制产生鼠IFN-γ或IL-17的γδT细胞的库大小。
2. Cutting Edge: Adaptive Versus Innate Receptor Signals Selectively Control the Pool Sizes of Murine IFN-γ– or IL-17–Producing γδ T Cells upon Infection [J] . Julie C. Ribot, Miguel Chaves-Ferreira, Francisco d’Orey, The journal of immunology . 2010 ,第11期

机译：前沿：自适应对先天受体信号选择性控制感染小鼠的产生IFN-γ或IL-17的γδT细胞的库大小
3. Cutting Edge: Adaptive Versus Innate Receptor Signals Selectively Control the Pool Sizes of Murine IFN-γ– or IL-17–Producing γδ T Cells upon Infection [J] . Julie C. Ribot, Miguel Chaves-Ferreira, Francisco d’Orey, The journal of immunology . 2010 ,第11期

机译：前沿：自适应对先天受体信号选择性控制感染小鼠的产生IFN-γ或IL-17的γδT细胞的库大小
4. A variable step-size adaptive noise canceller using signal to noise ratio as the controlling factor [C] . Ramadan, Z., Poularikas, . 2004

机译：以信噪比为控制因子的可变步长自适应噪声消除器
5. Cutting Edge: Adaptive Versus Innate Receptor Signals Selectively Control the Pool Sizes of Murine IFN-γ– or IL-17–Producing γδ T Cells upon Infection [O] . Julie C. Ribot, Miguel Chaves-Ferreira, Francisco d’Orey, -1

机译：切削刃：自适应对战先天受体信号选择性地控制的鼠IFN-γ-或的池大小IL-17生产γδ在感染性T细胞
6. Cutting Edge: Adaptive Versus Innate Receptor Signals Selectively Control the Pool Sizes of Murine IFN-gamma- or IL-17-Producing gamma delta T Cells upon Infection [O] . Ribot, Julie C., Chaves-Ferreira, Miguel, d&apos, 2010

机译：尖端：自适应对先天受体信号选择性地控制感染后产生小鼠IFN-γ-或IL-17的γ-δT细胞的库大小

Cutting edge: adaptive versus innate receptor signals selectively control the pool sizes of murine IFN-gamma- or IL-17-producing gammadelta T cells upon infection.

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