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树突状细胞上OX40配体的表达在体内作为一种共刺激而非极化信号,以实现最佳的Th2启动和记忆诱导。

Dendritic cell expression of OX40 ligand acts as a costimulatory, not polarizing, signal for optimal Th2 priming and memory induction in vivo.

作者信息

Jenkins Stephen J, Perona-Wright Georgia, Worsley Alan G F, Ishii Naoto, MacDonald Andrew S

机构信息

Institute of Immunology and Infection Research, School of Biological Sciences, University of Edinburgh, Edinburgh, United Kingdom.

出版信息

J Immunol. 2007 Sep 15;179(6):3515-23. doi: 10.4049/jimmunol.179.6.3515.

Abstract

Costimulatory cross-talk can occur at multiple cellular levels to potentiate expansion and polarization of Th responses. Although OX40L ligand (OX40L) is thought to play a key role in Th2 development, the critical cellular source of this molecule has yet to be identified. In this study, we demonstrate that OX40L expression by the initiating dendritic cell (DC) is a fundamental requirement for optimal induction of primary and memory Th2 responses in vivo. Analysis of the kinetics of the residual Th2 response primed by OX40L-deficient DC suggested a failure to stimulate appropriate expansion and/or survival of T cells, rather than an inability to polarize per se. The dependence upon OX40L was predominantly due to the provision of signaling through OX40 rather than retrograde signaling to the DC. Mechanistically, impaired Th2 priming in the absence of OX40L was not due to exaggerated regulation because there was no evidence of increased expansion or function of regulatory cell populations, suppression through IL-10 production, or hyporesponsiveness to secondary challenge. These data define a critical role for DC-derived OX40L in the induction and development of Th2 responses in vivo.

摘要

共刺激相互作用可在多个细胞水平发生,以增强Th反应的扩增和极化。尽管OX40L配体(OX40L)被认为在Th2细胞发育中起关键作用,但该分子的关键细胞来源尚未确定。在本研究中,我们证明起始树突状细胞(DC)表达OX40L是体内最佳诱导原发性和记忆性Th2反应的基本要求。对OX40L缺陷型DC引发的残余Th2反应动力学的分析表明,未能刺激T细胞进行适当的扩增和/或存活,而不是无法进行极化本身。对OX40L的依赖性主要是由于通过OX40提供信号,而不是向DC的逆向信号。从机制上讲,在没有OX40L的情况下Th2引发受损并非由于过度调节,因为没有证据表明调节细胞群体的扩增或功能增加、通过IL-10产生进行抑制或对二次刺激反应低下。这些数据确定了DC衍生的OX40L在体内Th2反应的诱导和发育中的关键作用。

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