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类视黄醇对用重氮丝氨酸处理的大鼠胰腺和肝脏致癌作用的不同影响。

Divergent effects of retinoids on pancreatic and liver carcinogenesis in azaserine-treated rats.

作者信息

Longnecker D S, Kuhlmann E T, Curphey T J

出版信息

Cancer Res. 1983 Jul;43(7):3219-25.

PMID:6601985
Abstract

Chemoprevention by synthetic retinoids of the progression of carcinomas of the pancreas induced in rats by azaserine was evaluated. Lewis rats were given five weekly injections of azaserine, 30 mg/kg, while being fed a chow diet. Two weeks after completion of carcinogen treatment, groups of rats were fed the chow diet supplemented with four different retinoids at the level of 0.5 to 2 mmol/kg of diet for 1 year. The incidence of pancreatic and other neoplasms was determined by autopsy and histological study. The incidence of localized pancreatic carcinoma among male and female non-retinoid-treated controls was 25 and 17%, respectively. No invasive or metastatic carcinomas were found in the control group. The combined incidence of localized and invasive pancreatic carcinomas among male and female rats treated with retinoids was: N-(4-pivaloyloxyphenyl)retinamide, 4 and 0%; N-(2-hydroxypropyl)retinamide, 14 and 6%; N-(3-hydroxypropyl)retinamide, 16 and 4%; and N-(2,3-dihydroxypropyl)retinamide, 12 and 6%. High- and low-dose groups are combined in this summary of data. Thus, there was a trend towards fewer pancreatic carcinomas among all retinoid-treated groups. The reduction in incidence was significant in both male and female rat groups given N-(4-pivaloyloxyphenyl)retinamide and N-(2,3-dihydroxypropyl)retinamide. The principal evidence of retinoid toxicity was growth failure, which was most severe in animals treated with N-(4-pivaloyloxyphenyl)retinamide, and testicular atrophy, which was most severe among male animals treated with N-(3-hydroxypropyl)retinamide. Among the females, groups treated with three of the four retinoids showed a dose-related increase in incidence of hepatocellular carcinomas. Since the retinoids were fed after the completion of exposure to the carcinogen, the effects on both pancreatic and liver carcinogenesis were exerted during the postinitiation phase of carcinogenesis.

摘要

评估了合成类视黄醇对大鼠中由偶氮丝氨酸诱导的胰腺癌进展的化学预防作用。给Lewis大鼠每周注射5次30mg/kg的偶氮丝氨酸,同时喂以普通饲料。致癌物处理完成两周后,将大鼠分组,喂以添加了四种不同类视黄醇的普通饲料,添加水平为0.5至2mmol/kg饲料,持续1年。通过尸检和组织学研究确定胰腺及其他肿瘤的发生率。在未接受类视黄醇处理的雄性和雌性对照组中,局部胰腺癌的发生率分别为25%和17%。对照组中未发现侵袭性或转移性癌。接受类视黄醇处理的雄性和雌性大鼠中局部和侵袭性胰腺癌的合并发生率为:N-(4-新戊酰氧基苯基)视黄酰胺,4%和0%;N-(2-羟丙基)视黄酰胺,14%和6%;N-(3-羟丙基)视黄酰胺,16%和4%;N-(2,3-二羟丙基)视黄酰胺,12%和6%。在此数据总结中,高剂量组和低剂量组合并。因此,在所有接受类视黄醇处理的组中,胰腺癌的数量有减少的趋势。给予N-(4-新戊酰氧基苯基)视黄酰胺和N-(2,3-二羟丙基)视黄酰胺的雄性和雌性大鼠组中,发生率的降低具有显著性。类视黄醇毒性的主要证据是生长迟缓,在用N-(4-新戊酰氧基苯基)视黄酰胺处理的动物中最为严重,以及睾丸萎缩,在用N-(3-羟丙基)视黄酰胺处理的雄性动物中最为严重。在雌性动物中,接受四种类视黄醇中三种处理的组肝细胞癌发生率呈剂量相关增加。由于类视黄醇是在接触致癌物后喂食的,其对胰腺癌和肝癌发生的影响是在致癌作用的启动后阶段发挥的。

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