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Mitochondrial dysfunction, persistently elevated levels of reactive oxygen species and radiation-induced genomic instability: a review

机译:线粒体功能障碍,活性氧水平持续升高和辐射引起的基因组不稳定:综述

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摘要

Radiation-induced genomic instability (RIGI) challenges the long-standing notion that radiation's effects derive solely from nuclear impact. In RIGI it is the unirradiated progeny that can display phenotypic changes at delayed times after irradiation of the parental cell. RIGI might well provide the driving force behind the development of radiation-induced tumorigenesis as most cancer cells even in pre-neoplastic states display multiple genetic alterations. Thus, understanding RIGI may help elucidate the mechanisms underlying radiation-induced carcinogenesis. One characteristic of clones of genetically unstable cells is that many exhibit persistently increased levels of reactive oxygen species (ROS). Furthermore, oxidants enhance and antioxidants diminish radiation-induced instability. However, much about the mechanisms behind the initiation and perpetuation of RIGI remains unknown and we examine the evidence for the hypothesis that oxidative stress and mitochondrial dysfunction may be involved in perpetuating the unstable phenotype in some cell clones surviving ionizing radiation.
机译:辐射诱发的基因组不稳定性(RIGI)挑战了一个长期存在的观念,即辐射的影响完全来自核影响。在RIGI中,未照射的后代可以在亲代细胞照射后的延迟时间显示表型变化。 RIGI可能会提供辐射诱发的肿瘤发生发展背后的驱动力,因为即使在肿瘤形成前的状态下,大多数癌细胞也表现出多种遗传改变。因此,了解RIGI可能有助于阐明辐射诱导的致癌作用的潜在机制。基因不稳定细胞克隆的一个特征是,许多克隆表现出持续增加的活性氧水平(ROS)。此外,氧化剂增强,抗氧化剂减少辐射引起的不稳定性。然而,RIGI的启动和持久化背后的许多机制仍是未知的,我们研究了以下假设的证据:氧化应激和线粒体功能障碍可能与某些在电离辐射中幸存的细胞克隆中的不稳定表型持久化有关。

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  • 来源
    《Mutagenesis》 |2006年第6期|361-367|共7页
  • 作者单位

    Graduate Program in Molecular and Cell Biology University of Maryland Baltimore 108 North Greene Street BRF Room 110C Baltimore MD 21201 USA;

    Radiation Oncology Research Laboratory 655 West Baltimore Street Baltimore MD 21201 USA;

    Marlene and Stewart Greenebaum Cancer Center University of Maryland School of Medicine 655 West Baltimore Street Baltimore MD 21201 USA;

    Department of Anesthesiology University of Maryland School of Medicine 685 West Baltimore Street MSTF 5–34 Baltimore MD 21201 USA;

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