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黄曲霉毒素 A 的致突变性:碳连接的 C8-脱氧鸟苷加合物的作用?

Mutagenicity of Ochratoxin A: Role for a Carbon-Linked C8-Deoxyguanosine Adduct?

机构信息

Departments of Chemistry and Toxicology, University of Guelph , Guelph, Ontario, Canada N1G 2W1.

Department of Chemistry & Biochemistry, University of Lethbridge , Lethbridge, Alberta, Canada T1K 3M4.

出版信息

J Agric Food Chem. 2017 Aug 23;65(33):7097-7105. doi: 10.1021/acs.jafc.6b03897. Epub 2016 Nov 15.

Abstract

Ochratoxin A (OTA) is a fungal toxin that is considered to be a potent kidney carcinogen in rodent models. The toxin produces double strand breaks and has a propensity for deletions, single-base substitutions, and insertions. The toxin reacts covalently with DNA to afford a C8-2'-deoxyguanosine carbon-linked adduct (OT-dG) as the major lesion in animal tissues. Incorporation of model C-linked C8-aryl-dG adducts into the G3 site of the NarI sequence demonstrates a tendency to induce base substitutions and deletion mutations in primer extension assays using model polymerases. The degree of misincorporation induced by the C-linked C8-dG adducts correlates with an ability to adopt the promutagenic syn conformation within the NarI duplex as predicted by molecular dynamics (MD) simulations. MD simulations of the OT-dG adduct within the NarI duplex predict an even greater degree of conformational flexibility, suggesting enhanced in vitro mutagenicity compared to the simpler model C-linked C8-dG adducts. Together these findings support the role of OT-dG in promoting OTA-mediated mutagenicity and carcinogenicity in animal studies.

摘要

赭曲霉毒素 A(OTA)是一种真菌毒素,被认为是啮齿动物模型中的一种强效肾脏致癌物质。该毒素会产生双链断裂,并具有缺失、单碱基取代和插入的倾向。该毒素与 DNA 发生共价反应,在动物组织中形成主要病变物 C8-2'-脱氧鸟苷碳键加合物(OT-dG)。将模型 C 连接的 C8-芳基-dG 加合物掺入 NarI 序列的 G3 位点,在使用模型聚合酶进行的引物延伸测定中,证明了诱导碱基取代和缺失突变的趋势。C 连接的 C8-dG 加合物诱导的错误掺入程度与分子动力学(MD)模拟预测的 NarI 双链体中诱发生物突变的 syn 构象的能力相关。在 NarI 双链体中 OT-dG 加合物的 MD 模拟预测出更高程度的构象灵活性,表明与更简单的模型 C 连接的 C8-dG 加合物相比,体外致突变性增强。这些发现共同支持了 OT-dG 在促进动物研究中 OTA 介导的致突变性和致癌性中的作用。

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