CD4+ T cells contain early extrapulmonary tuberculosis (TB) dissemination and rapid TB progression and sustain multieffector functions of CD8+ T and CD3- lymphocytes: mechanisms of CD4+ T cell immunity.

Shuyu Yao; Dan Huang; Crystal Y Chen; Lisa Halliday; Richard C Wang; Zheng W Chen

首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >CD4+ T cells contain early extrapulmonary tuberculosis (TB) dissemination and rapid TB progression and sustain multieffector functions of CD8+ T and CD3- lymphocytes: mechanisms of CD4+ T cell immunity.

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CD4+ T cells contain early extrapulmonary tuberculosis (TB) dissemination and rapid TB progression and sustain multieffector functions of CD8+ T and CD3- lymphocytes: mechanisms of CD4+ T cell immunity.

机译：CD4 + T细胞包含早期的肺外结核（TB）传播和快速的TB进展，并维持CD8 + T和CD3-淋巴细胞的多效应子功能：CD4 + T细胞免疫的机制。

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The possibility that CD4(+) T cells can act as "innate-like" cells to contain very early Mycobacterium tuberculosis dissemination and function as master helpers to sustain multiple effector functions of CD8(+) T cells and CD3(-) lymphocytes during development of adaptive immunity against primary tuberculosis (TB) has not been demonstrated. We showed that pulmonary M. tuberculosis infection of CD4-depleted macaques surprisingly led to very early extrapulmonary M. tuberculosis dissemination, whereas CD4 deficiency clearly resulted in rapid TB progression. CD4 depletion during M. tuberculosis infection revealed the ability of CD8(+) T cells to compensate and rapidly differentiate to Th17-like/Th1-like and cytotoxic-like effectors, but these effector functions were subsequently unsustainable due to CD4 deficiency. Whereas CD3(-) non-T lymphocytes in the presence of CD4(+) T cells developed predominant Th22-like and NK-like (perforin production) responses to M. tuberculosis infection, CD4 depletion abrogated these Th22-/NK-like effector functions and favored IL-17 production by CD3(-) lymphocytes. CD4-depleted macaques exhibited no or few pulmonary T effector cells constitutively producing IFN-γ, TNF-α, IL-17, IL-22, and perforin at the endpoint of more severe TB, but they presented pulmonary IL-4(+) T effectors. TB granulomas in CD4-depleted macaques contained fewer IL-22(+) and perforin(+) cells despite the presence of IL-17(+) and IL-4(+) cells. These results implicate a previously unknown innate-like ability of CD4(+) T cells to contain extrapulmonary M. tuberculosis dissemination at very early stage. Data also suggest that CD4(+) T cells are required to sustain multiple effector functions of CD8(+) T cells and CD3(-) lymphocytes and to prevent rapid TB progression during M. tuberculosis infection of nonhuman primates.

机译：CD4（+）T细胞可以充当“先天性”细胞以包含非常早的结核分枝杆菌传播并起主要辅助作用的可能性，以在发育过程中维持CD8（+）T细胞和CD3（-）淋巴细胞的多种效应子功能尚未证明对原发性肺结核（TB）具有适应性免疫力。我们显示，肺结核分枝杆菌感染CD4减少的猕猴令人惊讶地导致了非常早的肺外结核分枝杆菌的传播，而CD4缺乏显然导致了结核病的快速发展。结核分枝杆菌感染期间的CD4耗竭揭示了CD8（+）T细胞补偿并迅速分化为Th17样/ Th1样和细胞毒性样效应子的能力，但由于CD4缺乏，这些效应子功能随后难以维持。在存在CD4（+）T细胞的情况下，CD3（-）非T淋巴细胞对结核分枝杆菌感染发展出主要的Th22-like和NK-like（穿孔素产生）反应，而CD4耗竭则废除了这些Th22- / NK-like效应子。的功能，并有利于CD3（-）淋巴细胞产生IL-17。耗竭CD4的猕猴在更严重的TB终点没有或仅有很少的肺T效应细胞组成性地产生IFN-γ，TNF-α，IL-17，IL-22和穿孔素，但它们呈现出肺IL-4（+）。 T效应器。尽管存在IL-17（+）和IL-4（+），但CD4缺失的猕猴中的TB肉芽肿包含较少的IL-22（+）和穿孔素（+）细胞。这些结果暗示了CD4（+）T细胞在非常早期阶段就含有肺外结核分枝杆菌传播的先前未知的先天样能力。数据还表明，需要CD4（+）T细胞来维持CD8（+）T细胞和CD3（-）淋巴细胞的多种效应子功能，并防止在非人灵长类动物的结核分枝杆菌感染期间快速的TB进展。

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《The Journal of Immunology: Official Journal of the American Association of Immunologists》 |2014年第5期|共13页
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Shuyu Yao; Dan Huang; Crystal Y Chen; Lisa Halliday; Richard C Wang; Zheng W Chen;
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1. CD4+ T cells contain early extrapulmonary tuberculosis (TB) dissemination and rapid TB progression and sustain multieffector functions of CD8+ T and CD3- lymphocytes: mechanisms of CD4+ T cell immunity. [J] . Shuyu Yao, Dan Huang, Crystal Y Chen, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2014,第5期

机译：CD4 + T细胞包含早期的肺外结核（TB）传播和快速的TB进展，并维持CD8 + T和CD3-淋巴细胞的多效应子功能：CD4 + T细胞免疫的机制。
2. CD4+ T Cells Contain Early Extrapulmonary Tuberculosis (TB) Dissemination and Rapid TB Progression and Sustain Multieffector Functions of CD8+ T and CD3? Lymphocytes: Mechanisms of CD4+ T Cell Immunity [J] . Shuyu Yao, Dan Huang, Crystal Y. Chen, The journal of immunology . 2014,第5期

机译：CD4 + T细胞含有早期的肺外结核（TB）传播和快速的TB进展，并维持CD8 + T和CD3的多效应子功能吗？淋巴细胞：CD4 + T细胞免疫的机制
3. Tim-3-Expressing CD4+ and CD8+ T Cells in Human Tuberculosis (TB) Exhibit Polarized Effector Memory Phenotypes and Stronger Anti-TB Effector Functions [J] . Boping Zhou, Crystal Y. Chen, Dan Huang, PLoS Pathogens . 2012,第11期

机译：在人类结核病（TB）中表达Tim-3的CD4 +和CD8 + T细胞表现出极化效应子记忆表型和更强的抗结核效应子功能
4. IMMUNIZATION OF DENDRITIC CELLS PULSED WITH PRRS VIRUS GP5 PROTEIN INDUCES CD4+ BUT NOT CD8+ T CELLS [C] . Nguyen-Dinh Quat, Jeongran Min, Jiwon Han, Congress ofthe International Pig Veterinary Society . 2008

机译：用PRRS病毒GP5蛋白脉冲树突细胞的免疫诱导CD4 +但不是CD8 + T细胞
5. Functional heterogeneity and helper roles of CD4+ T cells in antiviral immunity. [D] . Hu, Zhuting. 2015

机译：CD4 + T细胞在抗病毒免疫中的功能异质性和辅助作用。
6. CD4+ T cells are required to contain early extrathoracic TB dissemination and sustain multi-effector functions of CD8+ T and CD3− lymphocytes [O] . Shuyu Yao, Dan Huang, Crystal Y. Chen, -1

机译：需要CD4 + T细胞包含胸腔外结核的早期传播并维持CD8 + T和CD3-−淋巴细胞的多效应子功能
7. Tim-3-expressing CD4+ and CD8+ T cells in human tuberculosis (TB) exhibit polarized effector memory phenotypes and stronger anti-TB effector functions. [O] . Yueqin Qiu, Jianbo Chen, Hongying Liao, 2012

机译：表达Tim-3的人结核病（TB）中的CD4 +和CD8 + T细胞表现出极化的效应记忆表型和更强的抗TB效应子功能。

CD4+ T cells contain early extrapulmonary tuberculosis (TB) dissemination and rapid TB progression and sustain multieffector functions of CD8+ T and CD3- lymphocytes: mechanisms of CD4+ T cell immunity.

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