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下一代 DNA 损伤测序。

Next-generation DNA damage sequencing.

机构信息

Department of Health Sciences and Technology, ETH Zürich, Schmelzbergstrasse 9, 8092 Zürich, Switzerland.

出版信息

Chem Soc Rev. 2020 Oct 21;49(20):7354-7377. doi: 10.1039/d0cs00647e. Epub 2020 Sep 24.

Abstract

Cellular DNA is constantly chemically altered by exogenous and endogenous agents. As all processes of life depend on the transmission of the genetic information, multiple biological processes exist to ensure genome integrity. Chemically damaged DNA has been linked to cancer and aging, therefore it is of great interest to map DNA damage formation and repair to elucidate the distribution of damage on a genome-wide scale. While the low abundance and inability to enzymatically amplify DNA damage are obstacles to genome-wide sequencing, new developments in the last few years have enabled high-resolution mapping of damaged bases. Recently, a number of DNA damage sequencing library construction strategies coupled to new data analysis pipelines allowed the mapping of specific DNA damage formation and repair at high and single nucleotide resolution. Strikingly, these advancements revealed that the distribution of DNA damage is heavily influenced by chromatin states and the binding of transcription factors. In the last seven years, these novel approaches have revealed new genomic maps of DNA damage distribution in a variety of organisms as generated by diverse chemical and physical DNA insults; oxidative stress, chemotherapeutic drugs, environmental pollutants, and sun exposure. Preferred sequences for damage formation and repair have been elucidated, thus making it possible to identify persistent weak spots in the genome as locations predicted to be vulnerable for mutation. As such, sequencing DNA damage will have an immense impact on our ability to elucidate mechanisms of disease initiation, and to evaluate and predict the efficacy of chemotherapeutic drugs.

摘要

细胞 DNA 会不断受到外源性和内源性因素的化学改变。由于生命的所有过程都依赖于遗传信息的传递,因此存在多种生物过程来确保基因组的完整性。化学损伤的 DNA 与癌症和衰老有关,因此,绘制 DNA 损伤的形成和修复图谱以阐明全基因组范围内的损伤分布情况具有重要意义。虽然低丰度和无法酶促扩增 DNA 损伤是全基因组测序的障碍,但近年来的新发展使得对受损碱基进行高分辨率图谱绘制成为可能。最近,一些与新数据分析管道相结合的 DNA 损伤测序文库构建策略使得能够以高分辨率和单核苷酸分辨率对特定的 DNA 损伤形成和修复进行作图。引人注目的是,这些进展表明,DNA 损伤的分布受到染色质状态和转录因子结合的强烈影响。在过去的七年中,这些新方法揭示了各种化学和物理 DNA 损伤对不同生物体的 DNA 损伤分布的新基因组图谱;氧化应激、化疗药物、环境污染物和阳光照射。已经阐明了损伤形成和修复的首选序列,从而有可能确定基因组中持续存在的薄弱点,这些位置被预测为易发生突变的位置。因此,对 DNA 损伤进行测序将极大地提高我们阐明疾病起始机制的能力,并评估和预测化疗药物的疗效。

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