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首页> 外文期刊>Antioxidants and redox signalling >Oxidation-sensitive transcription factors and molecular mechanisms in the arterial wall.
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Oxidation-sensitive transcription factors and molecular mechanisms in the arterial wall.

机译:动脉壁中氧化敏感的转录因子和分子机制。

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Adaptation to various forms of cellular stress involves signal transduction into the cytoplasm and subsequently into the cellular nucleus, and ultimately alteration of gene regulation and expression. Increased oxidative stress, which is associated with increased production of reactive oxygen species and other radical species, plays a pivotal role in vascular dysfunction and contributes substantially to the structural and functional changes leading to vascular disease progression. Activation of oxidation-sensitive transcription factors and molecular mechanisms can be triggered in the systemic, tissue, cellular, and molecular environments, thereby affecting a multitude of pathophysiological events involved in the pathogenesis of atherosclerosis and other vascular diseases. Radicals per se also participate in the pathophysiological vascular response to shear stress and injury. Among the oxidation-sensitive transcription factors, important roles have been ascribed to nuclear factor-kappaB, c-Myc, and the peroxisome proliferator-activated receptor family. Regulation of nuclear events has also been recently proposed to involve corepressor and coactivator molecules. Identification of the genes that are involved in these processes has been facilitated by recent development of microarray chip techniques, which allow simultaneous evaluation of differential gene expression. As many of the transcription factors or their interactions are redox-regulated, antioxidant intervention may affect their bioactivity.
机译:适应各种形式的细胞应激涉及信号转导进入细胞质,然后转导进入细胞核,并最终改变基因调控和表达。氧化应激的增加与活性氧物质和其他自由基物质的产生有关,在血管功能障碍中起着关键作用,并在很大程度上导致导致血管疾病进展的结构和功能变化。氧化敏感的转录因子和分子机制的激活可以在全身,组织,细胞和分子环境中触发,从而影响动脉粥样硬化和其他血管疾病的发病机理中涉及的多种病理生理事件。自由基本身也参与对剪应力和损伤的病理生理血管反应。在氧化敏感的转录因子中,重要的作用已归因于核因子-κB,c-Myc和过氧化物酶体增殖物激活的受体家族。最近还提出了调节核事件的方法,涉及到corepressor和coactivator分子。最近,微阵列芯片技术的发展促进了参与这些过程的基因的鉴定,该技术允许同时评估差异基因的表达。由于许多转录因子或其相互作用均受氧化还原调节,因此抗氧化剂干预可能会影响其生物活性。

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