ENZYME INDUCERS EFFECT ON LIVER PRENEOPLASTIC LESIONS

酶诱导剂对肝脏癌前病变的影响

• 批准号: 2153480
• 负责人: David L Eaton
• 金额: $ 19.15万
• 依托单位: UNIVERSITY OF WASHINGTON
• 依托单位国家: 美国
• 财政年份: 1988
• 资助国家: 美国
• 起止时间: 1988-05-01 至 1995-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/2153480
• 关键词: DNA replication; acetylaminofluorene; aflatoxins; biotransformation; biphenyl compounds; carcinogenesis inhibitor; chemical binding; chemical carcinogen; chemical carcinogenesis; cocarcinogen; cytochrome P450; disease /disorder model; environment related neoplasm /cancer; enzyme induction /repression; estradiol; glucuronides; hepatectomy; hepatocellular carcinoma; hepatotoxin; hydroxylation; hyperplasia; in situ hybridization; isozymes; laboratory rat; liver disorder; microsomes; nutrition aspect of cancer; nutrition related tag; phenobarbital; preneoplastic state; testosterone; toxin metabolism; tumor promoters

Chemical carcinogenesis is a multi-step process which can be influenced by variety of exogenous and endogenous factors. Most studies examining the effects of environmental and dietary substances on the carcinogenic process have focused on changes in the first step - initiation. However, there is increasing evidence that dietary and environmental chemicals which are effective biotransformation enzyme inducers may also modify later stages of the carcinogenic process. It appears that many non-genotoxic carcinogens may act in this manner. Compared to our understanding of the role of enzyme induction in the initiation step of carcinogenesis, relatively little is known about the relationship between enzyme induction and post-initiation events such as tumor promotion and progression. It has been recognized for many years that the same enzyme system responsible for biotransformation of xenobiotics also metabolize endogenous substances, especially steroid hormones. It is also known that the intracellular concentration of a variety of endogenous hormones can substantially alter cell growth and differentiation, processes intimately involved in tumor promotion and progression. The long range objective of this study is to understand how environmental and dietary factors influence the development and progression of chemical carcinogenesis, especially "post-initiation" events such as tumor promotion and progression. The primary goal of this grant is to investigate whether there is a causal connection between the tumor promoting abilities of non-genotoxic "environmental" carcinogens and their ability to induce, or not induce, specific isoenzymes of cytochrome P-450 in different preneoplastic lesions and normal tissue. We intend to use two "short-term" altered foci / nodule models which vary in their responsiveness to induction of cytochromes P450: the widely used "Solt-Farber" model which uses DEN and AAF to induce foci and nodules (SF-HHNs), and an altered foci and nodule model produce with aflatoxin Bl. The specific aims of this study are to: I.Evaluate the mechanism(s) by which Solt-Farber nodules are stimulated to expand by short-term treatment with phenobarbital; 2. Determine whether other PBtype inducers such as 2,2',4,4'-tetrachlorobiphenyl and DDT, or 3-MC-type inducers such as 3,3',4,4'tetrachlorobiphenyl and TCDD, produce a similar dramatic expansion of SF-HHNs, and whether an inducer only acts on specific foci/nodule populations which have an altered "induction responsiveness" of specific P450s. 3. Determine: a) whether phenobarbital expansion of SF-HHN requires the presence normal levels of thyroid or sex hormones; b) whether SF-HHNs have more bound forms of hormones and/or their respective receptors; c) whether microsomal hydroxylation activities toward testosterone or estradiol, and deiodination and/or glucuronide conjugation activities toward T3 are lower in SF-HHNs than the surrounding tissue; 4. Determine the profile of alterations in specific cytochromes P-450 in SF-HHN, using immunohistology and in situ hybridization with specific antibodies and specific oligonucleotide probes.

化学致癌是一个可影响的多步骤过程

项目成果

Complementary DNA cloning, messenger RNA expression, and induction of alpha-class glutathione S-transferases in mouse tissues.

小鼠组织中互补 DNA 克隆、信使 RNA 表达和 α 类谷胱甘肽 S-转移酶的诱导。

• 发表时间: 1992
• 期刊: Cancer research
• 影响因子: 11.2
• 作者: Buetler,TM;Eaton,DL
• 通讯作者: Eaton,DL

Inhibition of cell proliferation by ciprofibrate in glutathione S-transferase P1-1-positive rat hepatic hyperplastic nodules.

环丙贝特对谷胱甘肽 S-转移酶 P1-1 阳性大鼠肝增生结节细胞增殖的抑制作用。

• 发表时间: 1994
• 期刊: Cancer research
• 影响因子: 11.2
• 作者: Chen,ZY;Liu,YF;He,CY;White,CC;Eaton,DL
• 通讯作者: Eaton,DL

Species susceptibility to aflatoxin B1 carcinogenesis: comparative kinetics of microsomal biotransformation.

物种对黄曲霉毒素 B1 致癌的易感性：微粒体生物转化的比较动力学。

• 发表时间: 1990
• 期刊: Cancer research
• 影响因子: 11.2
• 作者: Ramsdell,HS;Eaton,DL
• 通讯作者: Eaton,DL

Modification of aflatoxin B1 biotransformation in vitro and DNA binding in vivo by dietary broccoli in rats.

大鼠膳食西兰花对黄曲霉毒素 B1 体外生物转化和体内 DNA 结合的修饰。

• DOI: 10.1080/15287398809531209
• 发表时间: 1988
• 期刊: Journal of toxicology and environmental health
• 作者: Ramsdell,HS;Eaton,DL
• 通讯作者: Eaton,DL

Aflatoxin B1-induced rat hepatic hyperplastic nodules do not exhibit a site-specific mutation within the p53 gene.

• 发表时间: 1993
• 期刊: Cancer research
• 影响因子: 11.2
• 作者: J. Hulla;Zhi-Ying Chen;D. Eaton