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氧化应激抑制受刺激淋巴细胞中的转录因子活性。

Oxidative stress suppresses transcription factor activities in stimulated lymphocytes.

作者信息

Flescher E, Tripoli H, Salnikow K, Burns F J

机构信息

Department of Environmental Medicine, New York University Medical Center, Tuxedo 10987, USA.

出版信息

Clin Exp Immunol. 1998 May;112(2):242-7. doi: 10.1046/j.1365-2249.1998.00548.x.

Abstract

Effects of oxidative stress on stimulation-dependent signal transduction, leading to IL-2 expression, were studied. Purified quiescent human blood T lymphocytes were subjected to: (i) acute exposure to hydrogen peroxide; (ii) chronic exposure to hydrogen peroxide; and (iii) acute exposure to ionizing radiation. The cells were then stimulated for 6 h. DNA-binding activities (determined by the electrophoretic mobility shift assay) of three transcription factors: NFkappaB, AP-1 and NFAT, were abolished in the lymphocytes by all three modes of oxidative stress. The lymphocytes exhibited lipid peroxidation only upon exposure to the lowest level of hydrogen peroxide used (20 microM). All three modes of oxidative stress induced catalase activity in the lymphocytes. The only exception was hydrogen peroxide at 20 microM, which did not induce catalase activity. We conclude that: (i) suppression of specific transcription factor functions can potentially serve as a marker of exposure to oxidative stress and its effects on human lymphocytes; (ii) lipid peroxidation is only detectable in human lymphocytes upon exposure to weak oxidative stress which does not induce catalase activity; (iii) therefore, transcription factor DNA-binding activities are more sensitive to oxidative stress than lipid peroxidation.

摘要

研究了氧化应激对导致白细胞介素-2表达的刺激依赖性信号转导的影响。纯化的静止人血T淋巴细胞接受以下处理:(i) 急性暴露于过氧化氢;(ii) 慢性暴露于过氧化氢;以及(iii) 急性暴露于电离辐射。然后将细胞刺激6小时。通过电泳迁移率变动分析测定的三种转录因子NFκB、AP-1和NFAT的DNA结合活性在淋巴细胞中被所有三种氧化应激模式所消除。淋巴细胞仅在暴露于所用最低浓度的过氧化氢(20微摩尔)时才表现出脂质过氧化。所有三种氧化应激模式均诱导淋巴细胞中的过氧化氢酶活性。唯一的例外是20微摩尔的过氧化氢,它不诱导过氧化氢酶活性。我们得出以下结论:(i) 特定转录因子功能的抑制可能作为暴露于氧化应激及其对人淋巴细胞影响的标志物;(ii) 脂质过氧化仅在暴露于不诱导过氧化氢酶活性的弱氧化应激时在人淋巴细胞中可检测到;(iii) 因此,转录因子DNA结合活性对氧化应激比脂质过氧化更敏感。

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