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8-硝基鸟嘌呤,一种由活性氮物质引起的DNA硝化损伤产物:形成、存在及其在炎症和致癌作用中的影响。

8-nitroguanine, a product of nitrative DNA damage caused by reactive nitrogen species: formation, occurrence, and implications in inflammation and carcinogenesis.

作者信息

Ohshima Hiroshi, Sawa Tomohiro, Akaike Takaaki

机构信息

International Agency for Research on Cancer, Lyon, France.

出版信息

Antioxid Redox Signal. 2006 May-Jun;8(5-6):1033-45. doi: 10.1089/ars.2006.8.1033.

Abstract

The authors review studies on 8-nitroguanine (8-NO(2)-G) formed by reactions of guanine, guanosine, and 2 - deoxyguanosine, either free or in DNA or RNAwith reactive nitrogen species (RNS) generated from peroxynitrite, the myeloperoxidase-H(2)O(2)-nitrite system, and others. Use of antibodies against 8-NO(2)-G has revealed increased formation of 8-NO(2)-G in various pathological conditions, including RNA virus-induced pneumonia in mice, intrahepatic bile ducts of hamsters infected with the liver fluke Opisthorchis viverrini, and gastric mucosa of patients with Helicobacter pylori-induced gastritis. Immunoreactivity has been found in the cytosol as well as in the nucleus of inflammatory cells and epithelial cells in inflamed tissues, but not in normal tissues. 8- NO(2)-G in DNA is potentially mutagenic, yielding G:C to T:A transversion, possibly through its rapid depurination to form an apurinic site and/or miscoding with adenine. 8-NO(2)-G in RNA may interfere with RNA functions and metabolism. Nitrated guanine nucleosides and nucleotides in the nucleotide pool may contribute to oxidative stress via production of superoxide mediated by various reductases and may disturb or modulate directly various important enzymes such as GTP-binding proteins and cGMP-dependent enzymes. Further studies are warranted to establish the roles of 8-NO(2)-G in various pathophysiological conditions and inflammation-associated cancer.

摘要

作者综述了关于鸟嘌呤、鸟苷和2-脱氧鸟苷(无论是游离状态还是存在于DNA或RNA中)与过氧亚硝酸盐、髓过氧化物酶-H₂O₂-亚硝酸盐系统及其他物质产生的活性氮物种(RNS)反应生成8-硝基鸟嘌呤(8-NO₂-G)的研究。使用针对8-NO₂-G的抗体已揭示在各种病理状况下8-NO₂-G的生成增加,包括小鼠RNA病毒诱导的肺炎、感染肝吸虫华支睾吸虫的仓鼠肝内胆管以及幽门螺杆菌诱导的胃炎患者的胃黏膜。在发炎组织的炎性细胞和上皮细胞的细胞质以及细胞核中发现了免疫反应性,但在正常组织中未发现。DNA中的8-NO₂-G具有潜在致突变性,可能通过其快速脱嘌呤形成无嘌呤位点和/或与腺嘌呤错配,导致G:C到T:A的颠换。RNA中的8-NO₂-G可能会干扰RNA的功能和代谢。核苷酸池中的硝化鸟嘌呤核苷和核苷酸可能通过各种还原酶介导的超氧化物产生导致氧化应激,并可能直接干扰或调节各种重要酶,如GTP结合蛋白和cGMP依赖性酶。有必要进一步研究以确定8-NO₂-G在各种病理生理状况和炎症相关癌症中的作用。

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