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氨基酸、蛋白质和细胞裂解物介导的丙烯醛衍生的环状 1,N(2)-丙二脱氧鸟苷加合物的区域选择性形成。

Regioselective formation of acrolein-derived cyclic 1,N(2)-propanodeoxyguanosine adducts mediated by amino acids, proteins, and cell lysates.

机构信息

Department of Oncology, Lombardi Comprehensive Cancer Center, Georgetown University Medical School, 3800 Reservoir Road NW, Washington, DC 20057, USA.

出版信息

Chem Res Toxicol. 2012 Sep 17;25(9):1921-8. doi: 10.1021/tx3002252. Epub 2012 Aug 14.

Abstract

Acrolein (Acr) is a major component in cigarette smoke and a ubiquitous environmental pollutant. It is also formed as a product of lipid peroxidation. Following ring closure via the Michael addition, Acr modifies deoxyguanosine (dG) in DNA by forming cyclic 1,N(2)-propanodeoxyguanosine adducts (OHPdG). The reactions of Acr with dG yield, depending on the direction of ring closure, two regioisomers, α- and γ-OHPdG, in approximately equal amounts. However, previous (32)P-postlabeling studies showed that the γ isomers were detected predominantly in the DNA of rodent and human tissues. Because of the potential differential biological activity of the isomeric OHPdG adducts, it is important to confirm and study the chemical basis of the regioselective formation of γ isomers in vivo. In this study, it is confirmed that γ-OHPdG adducts are indeed the major isomers formed in vivo as evidenced by a LC-MS/MS method specifically developed for Acr-derived dG adducts. Furthermore, we have shown that the formation of γ-isomers is increased in the presence of amino-containing compounds, including amino acids, proteins, and cell lysates. A product of Acr and arginine that appears to mediate the regioselective formation of γ isomers was identified, but its structure was not fully characterized due to its instability. This study demonstrates that intracellular amino-containing compounds may influence the regiochemistry of the formation of OHPdG adducts and reveals a mechanism for the preferential formation of γ-OHPdG by Acr in vivo.

摘要

丙烯醛(Acr)是香烟烟雾中的主要成分,也是一种普遍存在的环境污染物。它也是脂质过氧化的产物。通过迈克尔加成进行环闭合后,Acr 通过形成环状 1,N(2)-丙酰脱氧鸟苷加合物(OHPdG)来修饰 DNA 中的脱氧鸟苷(dG)。Acr 与 dG 的反应根据环闭合的方向产生两种区域异构体,α-和 γ-OHPdG,其含量大致相等。然而,先前的(32)P-后标记研究表明,γ 异构体主要在啮齿动物和人类组织的 DNA 中检测到。由于异构体 OHPdG 加合物的潜在差异生物学活性,因此确认和研究体内 γ 异构体的区域选择性形成的化学基础非常重要。在这项研究中,通过专门为 Acr 衍生的 dG 加合物开发的 LC-MS/MS 方法证实,γ-OHPdG 加合物确实是体内形成的主要异构体。此外,我们已经表明,在存在含氨基的化合物(包括氨基酸、蛋白质和细胞裂解物)的情况下,γ-异构体的形成会增加。鉴定出似乎介导 γ-异构体区域选择性形成的 Acr 和精氨酸的产物,但由于其不稳定性,其结构未完全表征。这项研究表明,细胞内含氨基的化合物可能会影响 OHPdG 加合物形成的区域化学,并揭示了体内 Acr 优先形成 γ-OHPdG 的机制。

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