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4-氧代-2-烯醛的DNA加合物丰度,脂质过氧化衍生的高反应性基因毒素。

Abundance of DNA adducts of 4-oxo-2-alkenals, lipid peroxidation-derived highly reactive genotoxins.

作者信息

Kawai Yoshichika, Nuka Erika

机构信息

Department of Food Science, Graduate School of Biomedical Science, Tokushima University, Kuramoto-cho 3-18-15, Tokushima 770-8503, Japan.

出版信息

J Clin Biochem Nutr. 2018 Jan;62(1):3-10. doi: 10.3164/jcbn.17-90. Epub 2017 Dec 12.

Abstract

Reactive oxygen species and their reaction products can damage DNA to form mutagenic lesions. Among the reactive species, lipid peroxidation-derived aldehydes react with nucleobases and form bulky exocyclic adducts. Many types of aldehyde-derived DNA adducts have been characterized, identified and detected and , whereas relative quantitative and pathophysiological contributions of each adduct still remain unclear. In recent years, an abundant class of DNA adducts derived from 4-oxo-2-alkenals have been identified, in addition to classic aldehyde-derived adducts. The presence of 4-oxo-2-alkenal-derived DNA adducts associated with age-related diseases has been revealed in rodents and humans. studies have demonstrated that 4-oxo-2-alkenals, as compared with other classes of lipid peroxidation-derived aldehydes, are highly reactive with nucleobases. It has been generally recognized that 4-oxo-2-alkenals are generated through oxidative degradation of the corresponding 4-hydroperoxy-2-alkenals, homolytic degradation products of polyunsaturated fatty acid hydroperoxides. Our recent results have also shown an alternative pathway for the formation of 4-oxo-2-alkenals, in which 2-alkenals could undergo the metal-catalyzed autoxidation resulting in the formation of the corresponding 4-oxo-2-alkenals. This review summarizes the basis of the formation of lipid peroxidation-derived genotoxic aldehydes and their covalent adduction to nucleobases, especially focusing on the abundance of 4-oxo-2-alkenal-derived DNA adducts.

摘要

活性氧及其反应产物会损伤DNA,形成诱变损伤。在这些活性物质中,脂质过氧化衍生的醛与核碱基发生反应,形成体积较大的环外加合物。许多类型的醛衍生DNA加合物已得到表征、鉴定和检测,然而,每种加合物的相对定量和病理生理作用仍不清楚。近年来,除了经典的醛衍生加合物外,还鉴定出了一类丰富的源自4-氧代-2-烯醛的DNA加合物。在啮齿动物和人类中已发现与年龄相关疾病相关的4-氧代-2-烯醛衍生DNA加合物的存在。研究表明,与其他脂质过氧化衍生的醛相比,4-氧代-2-烯醛与核碱基的反应性很高。人们普遍认为,4-氧代-2-烯醛是通过相应的4-氢过氧-2-烯醛(多不饱和脂肪酸氢过氧化物的均裂降解产物)的氧化降解产生的。我们最近的研究结果还表明了一种形成4-氧代-2-烯醛的替代途径,即2-烯醛可发生金属催化的自氧化反应,生成相应的4-氧代-2-烯醛。本综述总结了脂质过氧化衍生的遗传毒性醛的形成基础及其与核碱基的共价加成,尤其关注4-氧代-2-烯醛衍生DNA加合物的丰度。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d191/5773838/3351f0e64020/jcbn17-90f01.jpg

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