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核因子-κB信号转导通路对次级淋巴器官发育的调控

Regulation of secondary lymphoid organ development by the nuclear factor-kappaB signal transduction pathway.

作者信息

Weih Falk, Caamaño Jorge

机构信息

Forschungszentrum Karlsruhe, Institute of Toxicology and Genetics, Karlsruhe, Germany.

出版信息

Immunol Rev. 2003 Oct;195:91-105. doi: 10.1034/j.1600-065x.2003.00064.x.

DOI:10.1034/j.1600-065x.2003.00064.x
PMID:12969313
Abstract

In primary lymphoid organs, such as thymus and bone marrow, B and T lymphocytes differentiate from lymphoid stem cells into mature albeit naïve effector cells. In contrast, secondary lymphoid organs, such as the spleen, lymph nodes, and Peyer's patches (PPs), provide an environment that enable lymphocytes to interact with each other, with accessory cells, and with antigens, resulting in the initiation of antigen-specific primary immune responses. Recently, the analysis of gene-knockout mice has shed light on the signaling pathways, cellular requirements, and molecular mechanisms involved in secondary lymphoid organ development. In particular, signals that converge on the nuclear factor-kappaB (NF-kappaB) pathway have been demonstrated to play an important role in both early developmental steps as well as maintenance of secondary lymphoid organ structures. Analysis of the histopathological changes in secondary lymphoid tissues of mice lacking individual Rel/NF-kappaB family members, upstream kinases, and receptors strongly indicates that activation of the recently described alternative NF-kappaB pathway by membrane-bound lymphotoxin, via p52-RelB heterodimers, plays a major role during initiation steps of secondary lymphoid organ development. Induction of the classical p50-RelA NF-kappaB activity, as exemplified by tumor necrosis factor receptor signaling, clearly also contributes, but seems to be involved primarily in later developmental step, such as the proper cellular and structural organization of B-cell follicles.

摘要

在胸腺和骨髓等初级淋巴器官中,B淋巴细胞和T淋巴细胞从淋巴干细胞分化为成熟但未致敏的效应细胞。相比之下,脾脏、淋巴结和派尔集合淋巴结(PPs)等次级淋巴器官提供了一个环境,使淋巴细胞能够相互作用,与辅助细胞相互作用,并与抗原相互作用,从而引发抗原特异性的初级免疫反应。最近,对基因敲除小鼠的分析揭示了次级淋巴器官发育所涉及的信号通路、细胞需求和分子机制。特别是,汇聚在核因子-κB(NF-κB)通路上的信号已被证明在早期发育步骤以及次级淋巴器官结构的维持中都发挥着重要作用。对缺乏单个Rel/NF-κB家族成员、上游激酶和受体的小鼠次级淋巴组织的组织病理学变化分析强烈表明,膜结合淋巴毒素通过p52-RelB异二聚体激活最近描述的替代NF-κB通路,在次级淋巴器官发育的起始步骤中起主要作用。以肿瘤坏死因子受体信号为例,经典的p50-RelA NF-κB活性的诱导显然也有贡献,但似乎主要参与后期发育步骤,如B细胞滤泡的正常细胞和结构组织。

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