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二乙基亚硝胺对大鼠肝脏和食管致癌作用的调节

Modulation of diethylnitrosamine carcinogenesis in rat liver and oesophagus.

作者信息

Balansky R M, Blagoeva P M, Mircheva Z I, De Flora S

机构信息

National Centre of Oncology, Sofia, Bulgaria.

出版信息

J Cell Biochem. 1994 Dec;56(4):449-54. doi: 10.1002/jcb.240560405.

Abstract

A series of 16 experiments, using a total of 2,000 BD6 rats, was designed in order to assess the ability of 8 individual agents or their combinations to modulate the liver and oesophageal carcinogenesis induced by multiple doses of diethylnitrosamine (DEN). Of the antioxidants tested, sodium selenite, ascorbic acid, and butylated hydroxytoluene generally exhibited protective effects on both types of tumors. In contrast, retinoic acid behaved as a promoter of DEN hepatocarcinogenesis, but this effect could be eliminated by its combination with either selenite or butylated hydroxytoluene. Caffeine and theophylline, when individually assayed, were devoid of significant protective effects, and the latter methylxanthine stimulated oesophageal tumorigenesis when administered after exposure to the carcinogen. Caffeine tended to decrease the multiplicity of liver tumors and potentiated the inhibitory effect of selenite in the liver. Irrespective of combination with caffeine, treatment with phenobarbital before each DEN injection tended to reduce the multiplicity of both liver and oesophageal tumors. On the other hand, the metabolic inhibitor diethyldithiocarbamate, given after each DEN injection, dramatically enhanced the incidence and multiplicity of oesophageal tumors. Thus, on the whole, modulation of DEN carcinogenesis varied depending on test agents, their combinations, dosages, treatment schedules, and target organ.

摘要

设计了一系列16项实验,总共使用2000只BD6大鼠,以评估8种单独试剂或其组合调节多剂量二乙基亚硝胺(DEN)诱导的肝脏和食管癌发生的能力。在所测试的抗氧化剂中,亚硒酸钠、抗坏血酸和丁基化羟基甲苯通常对两种类型的肿瘤均表现出保护作用。相比之下,视黄酸在DEN肝癌发生过程中起促进作用,但这种作用可通过其与亚硒酸盐或丁基化羟基甲苯联合使用而消除。单独检测时,咖啡因和茶碱没有显著的保护作用,并且后者这种甲基黄嘌呤在接触致癌物后给药时会刺激食管肿瘤发生。咖啡因倾向于降低肝脏肿瘤的数量,并增强亚硒酸盐在肝脏中的抑制作用。无论是否与咖啡因联合使用,在每次注射DEN之前用苯巴比妥治疗都倾向于减少肝脏和食管肿瘤的数量。另一方面,在每次注射DEN后给予代谢抑制剂二乙基二硫代氨基甲酸盐,会显著提高食管肿瘤的发生率和数量。因此,总体而言,DEN致癌作用的调节因测试试剂、其组合、剂量、治疗方案和靶器官而异。

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