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指导性细胞因子信号在树突状细胞谱系分化中的作用。

Instructive cytokine signals in dendritic cell lineage commitment.

机构信息

Institute for Research in Biomedicine (IRB), Bellinzona, Switzerland.

出版信息

Immunol Rev. 2010 Mar;234(1):32-44. doi: 10.1111/j.0105-2896.2009.00877.x.

DOI:10.1111/j.0105-2896.2009.00877.x
PMID:20193010
Abstract

Clarifying the signals that lead to dendritic cell (DC) development and identifying cellular intermediates on their way to DC differentiation are essential steps to understand the dynamic regulation of number, localization, and functionality of these cells. In the past decade, much knowledge on cytokines, transcription factors, and successive progenitors involved in steady-state and demand-adapted DC development was gained. From the stage of multipotent progenitors, DCs are generated from Flt3(+) intermediates, irrespective of lymphoid or myeloid commitment, making fms-related tyrosine kinase 3 ligand one of the major regulators for DC development. Additional key cytokines involved are granulocyte-macrophage colony-stimulating factor (GM-CSF) and M-CSF, with each being essential for particular DC subsets and leading to specific activation of downstream transcription factors. In this review, we seek to draw an integrative view on how instructive cytokine signals acting on intermediate progenitors might lead to the generation of specific DC subsets in steady-state and during inflammation. We hypothesize that the lineage potential of a progenitor might be determined by the set of cytokine receptors expressed that make it responsive to further receive lineage instructive signals. Commitment to a certain lineage might consequently occur when lineage-relevant cytokine receptors are further upregulated and others for alternative lineages are lost. Along this line, we emphasize the role that diverse microenvironments have in influencing the generation of DC subsets with specific functions throughout the body.

摘要

阐明导致树突状细胞 (DC) 发育的信号,并确定其向 DC 分化过程中的细胞中间产物,是理解这些细胞数量、定位和功能的动态调节的重要步骤。在过去的十年中,人们对参与稳态和需求适应的 DC 发育的细胞因子、转录因子和连续祖细胞有了更多的了解。从多能祖细胞阶段开始,无论淋巴样还是髓样定向,DC 都由 Flt3(+) 中间产物产生,这使得 fms 相关酪氨酸激酶 3 配体成为 DC 发育的主要调节因子之一。另外涉及的关键细胞因子是粒细胞-巨噬细胞集落刺激因子 (GM-CSF) 和 M-CSF,它们对特定的 DC 亚群都至关重要,并导致下游转录因子的特异性激活。在这篇综述中,我们试图综合考虑指导细胞因子信号作用于中间祖细胞如何导致稳态和炎症期间特定 DC 亚群的产生。我们假设祖细胞的谱系潜能可能由表达的细胞因子受体决定,这些受体使其对进一步接收谱系指导信号有反应。当与特定谱系相关的细胞因子受体进一步上调,而其他替代谱系的受体丢失时,就会发生向特定谱系的定向。沿着这条线,我们强调了不同的微环境在影响具有特定功能的 DC 亚群在全身生成中的作用。

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