N-乙酰联苯胺和N，N'-二乙酰联苯胺在体内和体外与大鼠和仓鼠肝脏DNA的结合

Binding of N-acetylbenzidine and N,N'-diacetylbenzidine to hepatic DNA of rat and hamster in vivo and in vitro.

作者信息

Kennelly J C, Beland F A, Kadlubar F F, Martin C N

出版信息

Carcinogenesis. 1984 Mar;5(3):407-12. doi: 10.1093/carcin/5.3.407.

DOI:10.1093/carcin/5.3.407

Abstract

Benzidine, a potent hepatocarcinogen in rodents, is readily metabolised to acetylated derivatives. In this study, the covalent binding of [3H-acetyl]N-acetylbenzidine and [3H-acetyl]N,N'-diacetylbenzidine to liver DNA in rats and hamsters was investigated. Binding to liver DNA of rats at 1 or 7 days after i.p. injection of N-acetylbenzidine was 2-fold higher than that observed in the liver DNA of hamsters which had been similarly treated. Analysis of enzymically hydrolysed DNA from both species indicated the presence of a single adduct which co-eluted with N-(deoxyguanosin-8-yl)-N'-acetylbenzidine. In vitro treatment of rat or hamster liver slices with N-acetylbenzidine also resulted in covalent binding to hepatic DNA and the identical DNA adduct was detected at levels comparable to that observed in vivo. When N,N'-diacetylbenzidine was injected i.p. into rats, a comparatively low level of binding to liver DNA was observed. Following enzymic hydrolysis, the major DNA adduct detected by h.p.l.c. analysis was again N-(deoxyguanosin-8-yl)-N'-acetylbenzidine accompanied by a small amount of N-(deoxyguanosin-8-yl)-N,N'-diacetylbenzidine. In vitro incubation of N,N'-diacetylbenzidine with rat liver slices resulted in DNA binding levels similar to that observed with N-acetylbenzidine. In contrast to what was found in vivo, N-(deoxyguanosin-8-yl)-N,N'-diacetylbenzidine was the major adduct detected in DNA from rat liver slices. These data suggest that both N-hydroxy-N'-acetylbenzidine and N-hydroxy-N,N'-diacetylbenzidine are proximate carcinogenic species of benzidine, with N-hydroxy-N'-acetylbenzidine the more important. The low level of N-(deoxyguanosin-8-yl)N,N'-diacetylbenzidine observed in vivo may be due to its rapid repair. Alternatively, N-sulphonyloxy-N,N'-diacetylbenzidine, which would produce this adduct on reaction with DNA, may be efficiently detoxified in vivo.

摘要

联苯胺是啮齿动物体内一种强效的肝癌致癌物，它很容易代谢为乙酰化衍生物。在本研究中，对[3H-乙酰基]N-乙酰基联苯胺和[3H-乙酰基]N,N'-二乙酰基联苯胺与大鼠和仓鼠肝脏DNA的共价结合进行了研究。腹腔注射N-乙酰基联苯胺后1天或7天，大鼠肝脏DNA的结合量比同样处理的仓鼠肝脏DNA中观察到的结合量高2倍。对两种动物经酶水解的DNA进行分析表明，存在一种单一加合物，其与N-(脱氧鸟苷-8-基)-N'-乙酰基联苯胺共洗脱。用N-乙酰基联苯胺对大鼠或仓鼠肝切片进行体外处理，也导致与肝DNA的共价结合，并且检测到相同的DNA加合物，其水平与体内观察到的相当。当将N,N'-二乙酰基联苯胺腹腔注射到大鼠体内时，观察到与肝脏DNA的结合水平相对较低。酶水解后，通过高效液相色谱分析检测到的主要DNA加合物再次是N-(脱氧鸟苷-8-基)-N'-乙酰基联苯胺，伴有少量N-(脱氧鸟苷-8-基)-N,N'-二乙酰基联苯胺。N,N'-二乙酰基联苯胺与大鼠肝切片进行体外孵育，导致的DNA结合水平与N-乙酰基联苯胺观察到的相似。与体内发现的情况相反，N-(脱氧鸟苷-8-基)-N,N'-二乙酰基联苯胺是大鼠肝切片DNA中检测到的主要加合物。这些数据表明，N-羟基-N'-乙酰基联苯胺和N-羟基-N,N'-二乙酰基联苯胺都是联苯胺的直接致癌物种，其中N-羟基-N'-乙酰基联苯胺更为重要。在体内观察到的低水平N-(脱氧鸟苷-8-基)N,N'-二乙酰基联苯胺可能是由于其快速修复。或者，与DNA反应会产生这种加合物的N-磺酰氧基-N,N'-二乙酰基联苯胺在体内可能被有效解毒。