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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Homeostasis of dendritic cells in lymphoid organs is controlled by regulation of their precursors via a feedback loop.
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Homeostasis of dendritic cells in lymphoid organs is controlled by regulation of their precursors via a feedback loop.

机译:淋巴器官中树突状细胞的稳态通过反馈回路调节其前体来控制。

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Dendritic cells (DCs) are key coordinators of the immune response, governing the choice between tolerance and immunity. Despite their importance, the mechanisms controlling the size of the DC compartment are largely unknown. Using a mouse model allowing continuous DC depletion, we show that maintenance of DC numbers in spleen is an active process mediated by Flt3-L-dependent regulation of precursor differentiation into DCs, rather than by changes in proliferation of the differentiated DCs. In particular, the frequency and differentiation potential of intrasplenic DC precursors increased in response to reduced DC numbers. Levels of Flt3-L, a cytokine required for DC differentiation, increased in the blood after DC depletion and returned to normal levels once the DC compartment filled up again. Our data suggest a feedback regulation of DC homeostasis whereby reduction of the DC pool size promotes differentiation of their precursors, via increased Flt3-L availability. This mechanism is different to those known for other immune cell types, such as the B- and T-cell compartments, whereby lymphopenia induces proliferation of already differentiated lymphocytes.
机译:树突状细胞(DC)是免疫反应的关键协调者,控制着耐受性和免疫力之间的选择。尽管具有重要意义,但控制DC隔室尺寸的机制仍然未知。使用允许连续耗竭DC的小鼠模型,我们表明维持脾脏DC数量是一个由Flt3-L依赖性前体分化为DC的调节所介导的活动过程,而不是由分化DC的增殖变化所介导。特别地,脾脏DC前体的频率和分化潜能响应于减少的DC数目而增加。 Flt3-L的水平是DC分化所需的细胞因子,在DC耗尽后血液中的水平会升高,一旦DC隔室再次充满,血液就会恢复正常水平。我们的数据表明DC动态平衡的反馈调节,从而通过增加Flt3-L的可用性减少DC库大小促进其前体的分化。这种机制与其他免疫细胞类型(例如B细胞和T细胞区室)已知的机制不同,在这种机制下,淋巴细胞减少症会诱导已经分化的淋巴细胞增殖。

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