Expression of the CDKN1A, MDM2, and ATM genes as a biomarker of the toxic effect of heavy metals (literature review)

D. Shaikhova, A. M. Amromina, I.A. Bereza
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Abstract

The development of new approaches enabling differentiation of a wide range of toxic effects can significantly improve risk assessment. To understand the response mechanisms at the molecular level, it is important to study the expression of genes responsible for DNA repair, since this process is one of the early responses to toxic effects. The purpose of the study was to summarize available data on the expression of repair CDKN1A, MDM2, and ATM genes associated with toxic effects of exposure to heavy metals. A systematic search was carried out to identify studies on a given topic in the PubMed, Web of Science, eLIBRARY and Google Scholar electronic databases using the following keywords: heavy metals, CDKN1A, MDM2, ATM, toxicity, DNA repair, and gene expression. The initial search for scientific publications was carried out independently by three authors; then all sources found were checked and compared to filter out duplicate papers. This review covers 50 literature sources. The analysis of toxicogenome studies allowed us to identify several genes for assessing heavy metal toxicity among a large number of candidate biomarkers. The most commonly considered genes are the p21/CDKN1A gene, the MDM2 proto-oncogene, and the ATM gene. Limitations. The review is limited to considering changes in the expression of only a small number of genes responsible for DNA repair. Conclusion. The expression of the above biomarker genes provides a detailed picture of the response of a biological system to hazardous exposures and can be used as part of the assessment of toxic effects.
CDKN1A、MDM2 和 ATM 基因的表达作为重金属毒性效应的生物标志物(文献综述)
开发能够区分各种毒性效应的新方法可以大大改善风险评估。要了解分子水平的反应机制,研究负责 DNA 修复的基因的表达非常重要,因为这一过程是对毒性效应的早期反应之一。本研究旨在总结与重金属暴露毒性效应相关的CDKN1A、MDM2和ATM修复基因表达的现有数据。在PubMed、Web of Science、eLIBRARY和Google Scholar电子数据库中对特定主题的研究进行了系统性检索,使用的关键词包括:重金属、CDKN1A、MDM2、ATM、毒性、DNA修复和基因表达。最初的科学出版物搜索由三位作者独立完成,然后对找到的所有来源进行检查和比较,以过滤重复的论文。本综述涵盖 50 篇文献资料。通过对毒性基因组研究的分析,我们从大量候选生物标志物中找出了几个用于评估重金属毒性的基因。最常考虑的基因是 p21/CDKN1A 基因、MDM2 原癌基因和 ATM 基因。局限性。该综述仅限于考虑少数负责 DNA 修复的基因的表达变化。结论。上述生物标记基因的表达可详细描述生物系统对危险暴露的反应,可作为毒性效应评估的一部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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