Center for Hematology and Regenerative Medicine (HERM), Department of Medicine Huddinge, Karolinska Institutet, Stockholm, Sweden.
Department of Microbiology, Tumor and Cell Biology (MTC), Karolinska Institutet, Stockholm, Sweden.
Sci Rep. 2016 Dec 1;6:37996. doi: 10.1038/srep37996.
During infection and inflammation, dendritic cells (DC) provide priming signals for natural killer (NK) cells via mechanisms distinct from their antigen processing and presentation functions. The influence of DC on resting NK cells, i.e. at steady-state, is less well studied. We here demonstrate that as early as 1 day after DC depletion, NK cells in naïve mice downregulated the NKG2D receptor and showed decreased constitutive phosphorylation of AKT and mTOR. Subsequently, apoptotic NK cells appeared in the spleen concomitant with reduced NK cell numbers. At 4 days after the onset of DC depletion, increased NK cell proliferation was seen in the spleen resulting in an accumulation of Ly49 receptor-negative NK cells. In parallel, NK cell responsiveness to ITAM-mediated triggering and cytokine stimulation dropped across maturation stages, suggestive of a functional deficiency independent from the homeostatic effect. A role for IL-15 in maintaining NK cell function was supported by a gene signature analysis of NK cell from DC-depleted mice as well as by in vivo DC transfer experiments. We propose that DC, by means of IL-15 transpresentation, are required to maintain not only homeostasis, but also function, at steady-state. These processes appear to be regulated independently from each other.
在感染和炎症期间,树突状细胞 (DC) 通过与抗原加工和呈递功能不同的机制为自然杀伤 (NK) 细胞提供初始信号。DC 对静息 NK 细胞(即在稳态下)的影响研究较少。我们在此证明,早在 DC 耗竭后 1 天,幼稚小鼠的 NK 细胞下调了 NKG2D 受体,并表现出 AKT 和 mTOR 的组成性磷酸化减少。随后,凋亡的 NK 细胞出现在脾脏中,同时 NK 细胞数量减少。在 DC 耗竭开始后的第 4 天,脾脏中观察到 NK 细胞增殖增加,导致 Ly49 受体阴性 NK 细胞的积累。同时,NK 细胞对 ITAM 介导的触发和细胞因子刺激的反应性在成熟阶段下降,提示存在独立于稳态效应的功能缺陷。通过对 DC 耗竭小鼠的 NK 细胞进行基因特征分析以及体内 DC 转移实验,支持了 IL-15 在维持 NK 细胞功能中的作用。我们提出,DC 通过 IL-15 的转染作用,不仅需要维持稳态,还需要维持 NK 细胞的功能。这些过程似乎是相互独立调节的。
