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由大鼠和小鼠肝脏微粒体及胞质溶胶介导的2-硝基芘代谢产生的主要DNA加合物C8修饰的脱氧鸟苷和C8修饰的脱氧腺苷的形成。

Formation of C8-modified deoxyguanosine and C8-modified deoxyadenosine as major DNA adducts from 2-nitropyrene metabolism mediated by rat and mouse liver microsomes and cytosols.

作者信息

Fu P P, Miller D W, Von Tungeln L S, Bryant M S, Lay J O, Huang K, Jones L, Evans F E

机构信息

National Center for Toxicological Research, Jefferson, Arkansas 72079.

出版信息

Carcinogenesis. 1991 Apr;12(4):609-16. doi: 10.1093/carcin/12.4.609.

Abstract

2-Nitropyrene, the geometric isomer of the most studied nitropolycyclic aromatic hydrocarbon (nitro-PAH), 1-nitropyrene, is an environmental contaminant detected in ambient air and a potent direct-acting mutagen. Its metabolic activation leading to the formation of DNA adducts was studied. The activated metabolite, N-hydroxy-2-aminopyrene, was prepared and reacted with calf thymus DNA. Upon enzymatic hydrolysis of the DNA, the resulting nucleosides were separated by HPLC, and the adducts were characterized by mass and proton NMR spectral analysis. Both N-(deoxyguanosin-8-yl)-2-aminopyrene and N-(deoxyadenosin-8-yl)-2-aminopyrene, in a 5:2 ratio, were identified. These adducts were then utilized as standards to identify the DNA adducts formed from reaction of [3H]2-nitropyrene with DNA mediated by liver microsomes and cytosols of mouse and rat. In all cases, both adducts were formed. The quantities of the two adducts formed in each system were: mouse liver microsomes (11.3 pmol [3H]2-nitropyrene/mg DNA), rat liver microsomes (23), mouse liver cytosol (11.4) and rat liver cytosol (5.1). Thus, these adducts were formed in highest yield from rat liver microsomes and the lowest from rat liver cytosol. The deoxyguanosine/deoxyadenosine adduct ratio was higher from rat and mouse liver microsomes (7.8:9.2) than from rat and mouse liver cytosols (2.5:3.1). Our results represent the first direct demonstration of a C8-deoxyadenosine adduct being formed as a major product from the reaction of a nitro-PAH metabolite with DNA.

摘要

2-硝基芘是研究最多的硝基多环芳烃(硝基-PAH)1-硝基芘的几何异构体,它是在环境空气中检测到的一种环境污染物,也是一种强效的直接作用诱变剂。对其导致DNA加合物形成的代谢活化过程进行了研究。制备了活化代谢物N-羟基-2-氨基芘,并使其与小牛胸腺DNA反应。DNA经酶水解后,所得核苷通过高效液相色谱法分离,加合物通过质谱和质子核磁共振光谱分析进行表征。鉴定出了比例为5:2的N-(脱氧鸟苷-8-基)-2-氨基芘和N-(脱氧腺苷-8-基)-2-氨基芘。然后将这些加合物用作标准品,以鉴定由[3H]2-硝基芘与小鼠和大鼠肝脏微粒体及胞质溶胶介导的DNA反应形成的DNA加合物。在所有情况下,两种加合物均形成。每个系统中形成的两种加合物的量分别为:小鼠肝脏微粒体(11.3 pmol [3H]2-硝基芘/mg DNA)、大鼠肝脏微粒体(23)、小鼠肝脏胞质溶胶(11.4)和大鼠肝脏胞质溶胶(5.1)。因此,这些加合物在大鼠肝脏微粒体中形成的产量最高,在大鼠肝脏胞质溶胶中形成的产量最低。大鼠和小鼠肝脏微粒体中的脱氧鸟苷/脱氧腺苷加合物比例(7.8:9.2)高于大鼠和小鼠肝脏胞质溶胶中的比例(2.5:3.1)。我们的结果首次直接证明了C8-脱氧腺苷加合物是硝基-PAH代谢物与DNA反应形成的主要产物。

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