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三氯乙烯在体外与DNA以及在体内与各种小鼠组织的RNA和DNA的相互作用。

Interactions of trichloroethylene with DNA in vitro and with RNA and DNA of various mouse tissues in vivo.

作者信息

Bergman K

出版信息

Arch Toxicol. 1983 Nov;54(3):181-93. doi: 10.1007/BF01239202.

Abstract

The covalent binding of 14C-1,1,2-trichloroethylene (14C-TRI) metabolites to calf thymus DNA in vitro and to RNA and DNA of mouse brain, lung, liver, kidney, spleen, pancreas, and testis after repeated i.p. injections has been studied. Hydrolysates of DNA reacted with 14C-TRI in vitro and hydrolysates of RNA and DNA from selected organs were separated on Aminex A6 for quantitation of alkylation products. The presence of 3,N4-etheno(deoxy)cytidine, 1,N6-etheno(deoxy)adenosine and 1,N6-ethenoadenine was investigated. No radioactivity could be registered in DNA incubated with 14C-TRI in the absence of liver microsomes. Covalent binding of 14C-TRI to DNA took place in the presence of liver microsomes from control mice. The binding was enhanced by 50% if liver microsomes from phenobarbital pretreated mice were used. The radioactivity in DNA reacted with 14C-TRI and microsomes from control mice was eluted in early fractions and together with thymidine. The same two peaks appeared on chromatography of DNA incubated with 14C-TRI and liver microsomes from phenobarbital pretreated mice. In addition, radioactivity was eluted together with 1,N6-ethenoadenine. Radioactivity was registered in RNA and DNA from all of the studied organs after i.p. injections of 14C-TRI. The radioactivity in RNA increased in the order brain less than testis less than pancreas less than kidney less than liver less than lung less than spleen. The radioactivity in DNA increased in the order brain less than kidney less than testis less than lung less than pancreas less than liver less than spleen. Aminex A6 chromatography revealed that the entire radioactivity in RNA from liver and kidney and in DNA from kidney, testis, lung, pancreas, and spleen was due to metabolic incorporation, particularly into guanine and adenine. This finding indicates that the C-C bond in TRI is split, with the formation of C1-fragments, during biotransformation in vivo. In liver DNA, the metabolic incorporation of radioactivity was insignificant. Instead, the dominant part of the radioactivity in liver DNA was eluted in early fractions. The elution profile of radioactivity in liver DNA gave no direct evidence of the formation of TRI-DNA adducts in vivo. No etheno-derivatives were identified as alkylation products of TRI in vivo, which is consistent with current theories of the metabolic fate of TRI.

摘要

研究了14C-1,1,2-三氯乙烯(14C-TRI)代谢产物在体外与小牛胸腺DNA以及在反复腹腔注射后与小鼠脑、肺、肝、肾、脾、胰腺和睾丸的RNA和DNA的共价结合。DNA水解产物在体外与14C-TRI反应,来自选定器官的RNA和DNA水解产物在Aminex A6上分离以定量烷基化产物。研究了3,N4-乙烯基(脱氧)胞苷、1,N6-乙烯基(脱氧)腺苷和1,N6-乙烯基腺嘌呤的存在情况。在没有肝微粒体的情况下,与14C-TRI孵育的DNA中未检测到放射性。在对照小鼠的肝微粒体存在下,14C-TRI与DNA发生共价结合。如果使用苯巴比妥预处理小鼠的肝微粒体,结合会增强50%。与14C-TRI和对照小鼠微粒体反应的DNA中的放射性在早期馏分中洗脱,并与胸苷一起洗脱。在用14C-TRI和苯巴比妥预处理小鼠的肝微粒体孵育的DNA色谱图上出现了相同的两个峰。此外,放射性与1,N6-乙烯基腺嘌呤一起洗脱。腹腔注射14C-TRI后,在所有研究器官的RNA和DNA中均检测到放射性。RNA中的放射性按以下顺序增加:脑<睾丸<胰腺<肾<肝<肺<脾。DNA中的放射性按以下顺序增加:脑<肾<睾丸<肺<胰腺<肝<脾。Aminex A6色谱分析表明,肝和肾RNA以及肾、睾丸、肺、胰腺和脾DNA中的全部放射性是由于代谢掺入,特别是掺入鸟嘌呤和腺嘌呤。这一发现表明,在体内生物转化过程中,TRI中的C-C键断裂,形成C1片段。在肝DNA中,放射性的代谢掺入不明显。相反,肝DNA中放射性的主要部分在早期馏分中洗脱。肝DNA中放射性的洗脱图谱没有提供体内形成TRI-DNA加合物的直接证据。在体内未鉴定出乙烯基衍生物作为TRI的烷基化产物,这与目前关于TRI代谢命运的理论一致。

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