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吞噬细胞中活性氧的产生:原因、时机和部位?

ROS production in phagocytes: why, when, and where?

机构信息

1.INSERM U757, Bldg. 440, Rue des Adeles, F-91405 Orsay, France.

出版信息

J Leukoc Biol. 2013 Oct;94(4):657-70. doi: 10.1189/jlb.1012544. Epub 2013 Apr 22.

DOI:10.1189/jlb.1012544
PMID:23610146
Abstract

In the phagocytosis field, ROS production by the phagocyte NOX has been associated with pathogen killing for the last 50 years. Since the discovery of nonphagocyte NOX, numerous other roles for ROS production have been identified. Oxidative stress and ROS-mediated signaling have received much attention in recent years. Much lower concentrations of ROS may be required for signaling compared with microbial killing. Based on the discoveries in nonphagocytic cells, it became logical to look for ROS functions distinct from pathogen killing, even in phagocytes. ROS are now linked to various forms of cell death, to chemotaxis, and to numerous modifications of cellular processes, including the NOX itself. ROS functions are clearly concentration-dependent over a wide range of concentrations. How much is required for which function? Which species are required for how much time? Is ROS signaling only a side effect of bactericidal ROS production? One major obstacle to answer these questions is the difficulty of reliable quantitative ROS detection. Signal transduction often takes place on a subcellular scale over periods of seconds or minutes, so the detection methods need to provide appropriate time and space resolution. We present examples of local ROS production, decreased degradation, signaling events, and potentially ROS-sensitive functions. We attempt to illustrate the current limitations for quantitative spatiotemporal ROS detection and point out directions for ongoing development. Probes for localized ROS detection and for combined detection of ROS, together with protein localization or other cellular parameters, are constantly improved.

摘要

在吞噬作用领域,吞噬细胞的 NOX 产生的 ROS 与过去 50 年来的病原体杀伤有关。自发现非吞噬细胞的 NOX 以来,人们已经确定了 ROS 产生的许多其他作用。氧化应激和 ROS 介导的信号转导近年来受到了广泛关注。与微生物杀伤相比,信号转导可能需要更低浓度的 ROS。基于非吞噬细胞的发现,即使在吞噬细胞中,寻找与病原体杀伤不同的 ROS 功能也变得合乎逻辑。ROS 现在与各种形式的细胞死亡、趋化作用以及包括 NOX 本身在内的许多细胞过程的修饰有关。ROS 功能在广泛的浓度范围内明显依赖于浓度。哪种功能需要多少?哪种物种需要多少时间?ROS 信号转导是否仅仅是杀菌 ROS 产生的副作用?回答这些问题的一个主要障碍是可靠的定量 ROS 检测的难度。信号转导通常在亚细胞尺度上发生,持续几秒钟或几分钟,因此检测方法需要提供适当的时间和空间分辨率。我们展示了局部 ROS 产生、降解减少、信号事件和潜在的 ROS 敏感功能的例子。我们试图说明当前定量时空 ROS 检测的局限性,并指出正在进行的发展方向。用于局部 ROS 检测和 ROS 与蛋白质定位或其他细胞参数的联合检测的探针不断得到改进。

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