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病毒感染和成熟的人树突状细胞通过细胞膜结合的 TNF 和 IL-15 的协同作用激活自然杀伤细胞。

Virally infected and matured human dendritic cells activate natural killer cells via cooperative activity of plasma membrane-bound TNF and IL-15.

机构信息

Department of Pathology and Immunology, University of Pittsburgh, Hillman Cancer Center, 5117 Centre Ave., Pittsburgh, PA 15213, USA.

出版信息

Blood. 2010 Jul 29;116(4):575-83. doi: 10.1182/blood-2009-08-240325. Epub 2010 Apr 29.

Abstract

Recombinant adenovirus-engineered dendritic cells (Ad.DCs) are potent immunologic adjuvants of antiviral and anticancer vaccines. The effectiveness of Ad.DC-based vaccines may depend on the ability of Ad.DCs to crosstalk with natural killer (NK) cells and to activate, polarize, and bridge innate and adaptive immunity. We investigated, for the first time, whether and how human Ad.DCs activate NK cells, and compared the Ad.DC function with that of immature DCs and matured DCs (mDCs). We found that adenovirus transduction and lipopolysaccharide/interferon-gamma-induced maturation increased expression of transmembrane tumor necrosis factor (TNF) and trans-presented (trans) interleukin-15 (IL-15) on DCs, leading to enhanced NK cell activation without enhancing DC susceptibility to NK cell-mediated killing. This crosstalk enhanced NK cell CD69 expression, interferon-gamma secretion, proliferation, and antitumor activities, with Ad.DCs being significantly more effective than immature DCs, but less effective than mDCs. The Ad.DC and mDC crosstalk with NK cells was largely prevented by physical separation of DCs and NK cells, and neutralization of total TNF and IL-15, but not by selective sequestration of soluble TNF. These findings demonstrate that both Ad.DCs and mDCs can efficiently promote innate immune functions by activation of NK cells through the cooperative activities of tmTNF and trans-IL-15 mediated by cell-to-cell contact.

摘要

重组腺病毒工程化树突状细胞(Ad.DC)是抗病毒和抗癌疫苗的有效免疫佐剂。Ad.DC 疫苗的有效性可能取决于 Ad.DC 与自然杀伤(NK)细胞相互作用以及激活、极化和桥接先天和适应性免疫的能力。我们首次研究了人 Ad.DC 是否以及如何激活 NK 细胞,并比较了 Ad.DC 与未成熟 DC 和成熟 DC(mDC)的功能。我们发现腺病毒转导和脂多糖/干扰素-γ诱导的成熟增加了 DC 表面跨膜肿瘤坏死因子(TNF)和转呈(trans)白细胞介素-15(IL-15)的表达,导致 NK 细胞激活增强,而不增加 DC 对 NK 细胞介导杀伤的敏感性。这种细胞间相互作用增强了 NK 细胞 CD69 的表达、干扰素-γ的分泌、增殖和抗肿瘤活性,Ad.DC 比未成熟 DC 更有效,但比 mDC 效果差。通过物理分离 DC 和 NK 细胞以及中和总 TNF 和 IL-15 可以显著阻止 Ad.DC 和 mDC 与 NK 细胞的相互作用,但不能通过选择性隔离可溶性 TNF 来阻止。这些发现表明,Ad.DC 和 mDC 都可以通过细胞间接触介导的 tmTNF 和 trans-IL-15 的协同作用,通过激活 NK 细胞来有效促进先天免疫功能。

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