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Flt3 配体和树突状细胞在 NK 细胞稳态中的体内作用。

In vivo role of Flt3 ligand and dendritic cells in NK cell homeostasis.

机构信息

Department of Molecular Virology, The Ohio State University, Columbus, OH43210, USA.

出版信息

J Immunol. 2010 Mar 15;184(6):2769-75. doi: 10.4049/jimmunol.0900685. Epub 2010 Feb 8.

DOI:10.4049/jimmunol.0900685
PMID:20142363
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2924750/
Abstract

IL-15 is required for NK cell development and homeostasis in vivo. Because IL-15 is presented in trans via its high-affinity IL-15Ralpha-chain to cells expressing the IL-15Rbetagamma complex, we postulated that certain IL-15-bearing cells must be required for NK cell homeostasis. Using IL-15(WT/WT) and IL-15(-/-) mice, bone marrow chimeras with normal cellularity, and a selective depletion of CD11c(hi) dendritic cells (DCs), we demonstrate that ablation of the resting CD11c(hi) DC population results in a highly significant decrease in the absolute number of mature NK cells. In contrast, administration of Flt3 ligand increases the CD11c(hi) DC population, which, when expressing IL-15, significantly expands mature NK cells via enhanced survival and proliferation. In summary, a CD11c(hi) DC population expressing IL-15 is required to maintain NK cell homeostasis under conditions of normal cellularity and also is required to mediate Flt3 ligand-induced NK cell expansion in vivo.

摘要

IL-15 对于体内 NK 细胞的发育和稳态是必需的。因为 IL-15 通过其高亲和力的 IL-15Ralpha 链呈递,以与表达 IL-15Rbeta-gamma 复合物的细胞相互作用,所以我们推测某些携带 IL-15 的细胞必须是 NK 细胞稳态所必需的。使用 IL-15(WT/WT)和 IL-15(-/-)小鼠、具有正常细胞数量的骨髓嵌合体,以及对 CD11c(hi)树突状细胞 (DC)的选择性耗竭,我们证明静止的 CD11c(hi)DC 群体的消融会导致成熟 NK 细胞的绝对数量显著减少。相比之下,Flt3 配体的给药增加了 CD11c(hi)DC 群体,当表达 IL-15 时,通过增强的存活和增殖,显著扩增成熟 NK 细胞。总之,表达 IL-15 的 CD11c(hi)DC 群体是维持正常细胞数量下 NK 细胞稳态所必需的,并且也是体内 Flt3 配体诱导 NK 细胞扩增所必需的。

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本文引用的文献

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