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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >TLR2 engagement on dendritic cells promotes high frequency effector and memory CD4 T cell responses.
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TLR2 engagement on dendritic cells promotes high frequency effector and memory CD4 T cell responses.

机译:TLR2参与树突状细胞可促进高频效应子和记忆CD4 T细胞反应。

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摘要

Ligation of TLR by distinct pathogen components provides essential signals for T cell priming, although how individual TLR engagement affects primary and memory T cell responses is not well defined. In this study, we demonstrate distinct effects of TLR2 vs TLR4 engagement on primary and memory CD4 T cell responses due to differential effects on APC. Priming of influenza hemagglutinin (HA)-specific naive CD4 T cells with HA peptide and the TLR2 agonist Pam3CysK in vivo resulted in a high frequency of activated HA-specific CD4 T cells that predominantly produced IL-2 and IL-17, whereas priming with HA peptide and the TLR4 agonist LPS yielded a lower frequency of HA-specific CD4 T cells and predominant IFN-gamma producers. TLR2 agonist priming depended on TLR2 expression by APC, as wild-type CD4 T cells did not expand in response to peptide and Pam3CysK in TLR2-deficient hosts. TLR2-mediated priming also led to an increased frequency of Ag-specific memory CD4 T cells compared with TLR4 priming and mediated enhanced secondary responses to influenza challenge. Our results show that TLR engagement on APC influences both primary and secondary CD4 T cell responses, and suggest that long-term functional capacities of T cells are set by innate signals during early phases of an infection.
机译:尽管不同的TLR参与如何影响原代和记忆性T细胞反应,但通过不同的病原体成分​​连接TLR可为T细胞启动提供必要的信号。在这项研究中,由于对APC的影响不同,我们证明了TLR2与TLR4结合对原代和记忆CD4 T细胞反应的不同影响。在体内用HA肽和TLR2激动剂Pam3CysK引发流感血凝素(HA)特异性幼稚CD4 T细胞导致高频率激活的HA特异性CD4 T细胞活化,主要产生IL-2和IL-17。 HA肽和TLR4激动剂LPS产生的HA特异性CD4 T细胞和主要的IFN-γ产生者的频率较低。 TLR2激动剂引发取决于APC的TLR2表达,因为在TLR2缺陷型宿主中,野生型CD4 T细胞不会响应肽和Pam3CysK扩增。与TLR4引发相比,TLR2介导的引发还导致Ag特异性记忆CD4 T细胞的频率增加,并介导了对流感病毒激发的次级反应增强。我们的结果表明,TLR在APC上的参与会影响CD4 T细胞的初级和次级反应,并表明T细胞的长期功能能力是由感染早期的先天信号所决定的。

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