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醋酸视黄酯延迟给药对乳腺癌发生的影响。

Influence of delayed administration of retinyl acetate on mammary carcinogenesis.

作者信息

McCormick D L, Moon R C

出版信息

Cancer Res. 1982 Jul;42(7):2639-43.

PMID:7083156
Abstract

Administration of a dietary retinoid supplement beginning 1 week after carcinogen administration is highly effective in the inhibition of rat mammary carcinogenesis. A study was designed at two carcinogen dose levels to determine to what extent retinoid feeding can be delayed and retain its chemoprotective effect. In the high-dose experiment, groups of 30 virgin female Sprague-Dawley rats received a single i.v. dose of 50 mg N-methyl-N-nitrosourea (MNU) per kg body weight and were fed a dietary supplement of 328 mg retinyl acetate per kg diet beginning at 1, 4, or 8 weeks after MNU administration. In the low-dose experiment, groups of 50 rats received 25 mg MNU per kg, and the retinoid was begun at 1, 4, 8, 12, 16, or 20 weeks post-MNU. Controls at both dose levels received a placebo diet beginning 1 week after carcinogen treatment. At the high MNU dose, retinyl acetate was most effective in inhibition of carcinogenesis when treatment was begun 1 week after MNU administration. Delaying retinyl acetate feeding until 4 weeks post-MNU resulted in slightly reduced chemoprotective efficacy, while an 8-week delay caused a complement loss of anticancer activity. At the low MNU dose, delaying retinyl acetate administration for up to 12 weeks after MNU administration caused no loss of chemopreventive efficacy. A 16-week delay resulted in decreased anticancer activity, while retinoid treatment begun 20 weeks post-MNU had no effect on cancer induction. Retinoid administration can be delayed beyond 1 week and retain its activity against rat mammary carcinogenesis; the length of delay allowable without loss of activity is a function of tumor latency.

摘要

在致癌物给药1周后开始给予膳食类视黄醇补充剂,对抑制大鼠乳腺癌发生非常有效。设计了一项针对两种致癌物剂量水平的研究,以确定类视黄醇喂养可以延迟到何种程度并仍保持其化学保护作用。在高剂量实验中,每组30只处女雌性斯普拉格-道利大鼠静脉注射单次剂量为每千克体重50毫克的N-甲基-N-亚硝基脲(MNU),并在MNU给药后1、4或8周开始给予每千克饮食含328毫克醋酸视黄酯的膳食补充剂。在低剂量实验中,每组50只大鼠接受每千克25毫克的MNU,类视黄醇在MNU给药后1、4、8、12、16或20周开始给予。两个剂量水平的对照组在致癌物处理后1周开始接受安慰剂饮食。在高MNU剂量下,醋酸视黄酯在MNU给药后1周开始治疗时对抑制癌症发生最有效。将醋酸视黄酯喂养推迟到MNU给药后4周导致化学保护功效略有降低,而推迟8周则导致抗癌活性完全丧失。在低MNU剂量下,MNU给药后将醋酸视黄酯给药推迟长达12周不会导致化学预防功效丧失。推迟16周导致抗癌活性降低,而在MNU给药后20周开始的类视黄醇治疗对癌症诱导没有影响。类视黄醇给药可以推迟到1周以上并保持其对大鼠乳腺癌发生的活性;在不丧失活性的情况下允许的延迟长度是肿瘤潜伏期的函数。

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