Role of Mitochondrial Oxidant Generation in Endothelial Cell Responses to Hypoxia

Daryl P. Pearlstein, Mir H. Ali, P. Mungai, K. Hynes, B. Gewertz, P. Schumacker
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引用次数: 164

Abstract

Endothelial cells increase their secretion of the cytokine interleukin-6 (IL-6) during hypoxia, which then acts in an autocrine fashion to increase the permeability of cell monolayers. These responses are attenuated by antioxidants, suggesting that reactive oxygen species (ROS) participate in signaling in hypoxic endothelium. We tested whether mitochondria are responsible for these ROS in human umbilical vein endothelial cells exposed to hypoxia. Oxidation of the probe 2′, 7′-dichlorodihydrofluorescein to fluorescent dichlorofluorescein or the probe dihydroethidium was used to assess oxidant signaling, whereas permeability was assessed by using transendothelial electrical resistance. Hypoxia elicited increases in dichlorofluorescein and dihydroethidium fluorescence that were abrogated by the mitochondrial electron transport (ET) inhibitors rotenone (2 &mgr;mol/L) and diphenyleneiodonium (5 &mgr;mol/L). The same ET inhibitors also attenuated hypoxia-induced increases in nuclear factor-&kgr;B (NF-&kgr;B) activation, although they did not abrogate NF-&kgr;B activation in response to endotoxin (lipopolysaccharide). ET inhibition also abolished the hypoxia-induced increases in IL-6 mRNA expression, hypoxia-stimulated IL-6 secretion into the media, and the hypoxia-induced increases in transendothelial electrical resistance of human umbilical vein endothelial cell monolayers. By contrast, the above responses to hypoxia were not significantly affected by treatment with the NAD(P)H oxidase inhibitor apocynin (30 &mgr;mol/L), the xanthine oxidase inhibitor allopurinol (100 &mgr;mol/L), or the NO synthase inhibitor N-nitro-l-arginine (100 &mgr;mol/L). We conclude that ROS signals originating from the mitochondrial ET chain trigger the increase in NF-&kgr;B activation, the transcriptional activation of IL-6, the secretion of IL-6 into the cell culture media, and the increases in endothelial permeability observed during hypoxia.
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线粒体氧化剂生成在内皮细胞缺氧反应中的作用
内皮细胞在缺氧时增加其细胞因子白细胞介素-6 (IL-6)的分泌,然后以自分泌方式增加细胞单层的通透性。这些反应被抗氧化剂减弱,表明活性氧(ROS)参与缺氧内皮的信号传导。我们在暴露于缺氧的人脐静脉内皮细胞中测试了线粒体是否对这些ROS负责。探针2 ',7 ' -二氯二氢荧光素氧化为荧光二氯荧光素或探针二氢乙啶用于评估氧化信号,而渗透性通过经内皮电阻评估。缺氧引起二氯荧光素和二氢乙啶荧光增加,而线粒体电子传递(ET)抑制剂鱼藤酮(2 μ mol/L)和二苯乙酮(5 μ mol/L)消除了这种荧光。同样的ET抑制剂也能减弱缺氧诱导的核因子-&kgr;B (NF-&kgr;B)激活的增加,尽管它们不能消除内毒素(脂多糖)引起的NF-&kgr;B激活。ET抑制还消除了缺氧诱导的IL-6 mRNA表达升高、缺氧刺激IL-6分泌到介质中以及缺氧诱导的人脐静脉内皮细胞单层经内皮电阻升高。相比之下,NAD(P)H氧化酶抑制剂罗布麻碱(30 μ mol/L)、黄嘌呤氧化酶抑制剂别嘌呤醇(100 μ mol/L)和NO合成酶抑制剂n -硝基- L -精氨酸(100 μ mol/L)对上述缺氧反应没有显著影响。我们的结论是,来自线粒体ET链的ROS信号触发NF-&kgr;B激活的增加,IL-6的转录激活,IL-6分泌到细胞培养基中,以及在缺氧时观察到内皮通透性的增加。
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