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Orai-1 和 STIM-1 复合物控制人类树突状细胞成熟。

The Orai-1 and STIM-1 complex controls human dendritic cell maturation.

机构信息

EA 4245 Cellules Dendritiques, Immunomodulation et Greffes, Université François Rabelais, IFR-136 Agents Transmissibles et Infectiologie, UFR de Médecine, Tours, France.

出版信息

PLoS One. 2013 May 20;8(5):e61595. doi: 10.1371/journal.pone.0061595. Print 2013.

DOI:10.1371/journal.pone.0061595
PMID:23700407
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3659124/
Abstract

Ca(2+) signaling plays an important role in the function of dendritic cells (DC), the professional antigen presenting cells. Here, we described the role of Calcium released activated (CRAC) channels in the maturation and cytokine secretion of human DC. Recent works identified STIM1 and Orai1 in human T lymphocytes as essential for CRAC channel activation. We investigated Ca(2+) signaling in human DC maturation by imaging intracellular calcium signaling and pharmalogical inhibitors. The DC response to inflammatory mediators or PAMPs (Pathogen-associated molecular patterns) is due to a depletion of intracellular Ca(2+) stores that results in a store-operated Ca(2+) entry (SOCE). This Ca(2+) influx was inhibited by 2-APB and exhibited a Ca(2+)permeability similar to the CRAC (Calcium-Released Activated Calcium), found in T lymphocytes. Depending on the PAMPs used, SOCE profiles and amplitudes appeared different, suggesting the involvement of different CRAC channels. Using siRNAi, we identified the STIM1 and Orai1 protein complex as one of the main pathways for Ca(2+) entry for LPS- and TNF-α-induced maturation in DC. Cytokine secretions also seemed to be SOCE-dependent with profile differences depending on the maturating agents since IL-12 and IL10 secretions appeared highly sensitive to 2-APB whereas IFN-γ was less affected. Altogether, these results clearly demonstrate that human DC maturation and cytokine secretions depend on SOCE signaling involving STIM1 and Orai1 proteins.

摘要

钙离子信号在树突状细胞(DC)的功能中起着重要作用,DC 是专业的抗原呈递细胞。在这里,我们描述了钙释放激活(CRAC)通道在人 DC 成熟和细胞因子分泌中的作用。最近的研究在人 T 淋巴细胞中鉴定出 STIM1 和 Orai1 是 CRAC 通道激活所必需的。我们通过成像细胞内钙信号和药理学抑制剂研究了人 DC 成熟过程中的钙信号。DC 对炎症介质或 PAMPs(病原体相关分子模式)的反应是由于细胞内钙储存的耗竭,导致储存操纵的钙内流(SOCE)。这种钙内流被 2-APB 抑制,并表现出与 T 淋巴细胞中发现的 CRAC(钙释放激活钙)相似的钙通透性。根据使用的 PAMPs,SOCE 谱和幅度似乎不同,表明涉及不同的 CRAC 通道。使用 siRNAi,我们鉴定了 STIM1 和 Orai1 蛋白复合物作为 LPS 和 TNF-α诱导的 DC 成熟过程中钙内流的主要途径之一。细胞因子分泌似乎也依赖于 SOCE,因为不同的成熟剂具有不同的谱,因为 IL-12 和 IL10 分泌对 2-APB 高度敏感,而 IFN-γ 的影响较小。总之,这些结果清楚地表明,人 DC 的成熟和细胞因子分泌依赖于涉及 STIM1 和 Orai1 蛋白的 SOCE 信号。

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