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首页> 外文期刊>Environmental toxicology and pharmacology >Single-molecule telomere length characterization by optical mapping in nano-channel array: Perspective and review on telomere length measurement
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Single-molecule telomere length characterization by optical mapping in nano-channel array: Perspective and review on telomere length measurement

机译:纳米通道阵列中光学映射的单分子端粒长度特征:透视和对端粒长度测量的综述

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摘要

In humans, the telomere consists of tandem 5'TTAGGG3' DNA repeats on both ends of all 46 chromosomes. Telomere shortening has been linked to aging and age-related diseases. Similarly, telomere length changes have been associated with chemical exposure, molecular-level DNA damage, and tumor development. Telomere elongation has been associated to tumor development, caused due to chemical exposure and molecular-level DNA damage. The methods used to study these effects mostly rely on average telomere length as a biomarker. The mechanisms regulating subtelomere-speciflc and haplotype-specific telomere lengths in humans remain understudied and poorly understood, primarily because of technical limitations in obtaining these data for all chromosomes. Recent studies have shown that it is the short telomeres that are crucial in preserving chromosome stability. The identity and frequency of specific critically short telomeres potentially is a useful biomarker for studying aging, age-related diseases, and cancer. Here, we will briefly review the role of telomere length, its measurement, and our recent single-molecule telomere length measurement assay. With this assay, one can measure individual telomere lengths as well as identify their physically linked subtelomeric DNA. This assay can also positively detect telomere loss, characterize novel subtelomeric variants, haplotypes, and previously uncharacterized recombined subtelomeres. We will also discuss its applications in aging cells and cancer cells, highlighting the utility of the single molecule telomere length assay.
机译:在人类中,Teleromere由串联5'ttaggg3'DNA重复,在所有46染色体的两端重复。端粒缩短与老龄化和年龄相关的疾病有关。类似地,端粒长度变化与化学暴露,分子水平DNA损伤和肿瘤发育有关。端粒伸长率与肿瘤发育有关,由于化学暴露和分子水平DNA损伤而导致。用于研究这些效果的方法主要依赖于平均端粒长度作为生物标志物。调节人类中的子立体制细胞和单倍型端端粒长度的机制仍然被解读并且理解得不好,主要是因为获得所有染色体的这些数据时的技术限制。最近的研究表明,这是一种在保存染色体稳定性方面至关重要的短端粒。特定批判性短端粒的身份和频率可能是用于研究老化,年龄相关疾病和癌症的有用生物标志物。在这里,我们将简要审查端粒长度,测量和我们最近的单分子端粒长度测量测定的作用。通过该测定,可以测量单个端粒长度以及识别其物理连接的子细胞计DNA。该测定还可以肯定地检测端粒损失,表征新的亚细胞微调变体,单倍型和先前没有表征重组的子细胞。我们还将探讨其在老化细胞和癌细胞中的应用,突出了单分子端粒长度测定的效用。

著录项

  • 来源
    《Environmental toxicology and pharmacology》 |2021年第2期|103562.1-103562.10|共10页
  • 作者单位

    School of Biomedical Engineering Science and Health Systems Drexel University Philadelphia PA USA;

    School of Biomedical Engineering Science and Health Systems Drexel University Philadelphia PA USA;

    School of Biomedical Engineering Science and Health Systems Drexel University Philadelphia PA USA;

    Medical Diagnostic and Translational Sciences Old Dominion University Norfolk VA USA;

    School of Biomedical Engineering Science and Health Systems Drexel University Philadelphia PA USA Institute of Molecular Medicine and Infectious Disease School of Medicine Drexel University Philadelphia PA USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Telomere length; Optical mapping; Telomere dysfunction;

    机译:端粒长度;光学映射;端粒功能障碍;

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