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洛邦德 - 威斯塔大鼠实验性前列腺癌的预防与治疗。I. 雌二醇、双氢睾酮及去势的影响

Prevention and treatment of experimental prostate cancer in Lobund-Wistar rats. I. Effects of estradiol, dihydrotestosterone, and castration.

作者信息

Pollard M, Luckert P H, Snyder D

机构信息

Lobund Laboratory, University of Notre Dame, Indiana 46556.

出版信息

Prostate. 1989;15(2):95-103. doi: 10.1002/pros.2990150203.

Abstract

The Lobund-Wistar (L-W) rat is unique in its susceptibility to spontaneous and induced metastasizing prostate adenocarcinomas (PAs). A single IV inoculation of methylnitrosourea (MNU) produced PAs in 20% of L-W rats in 12 months. The combination of MNU plus two to seven slow-release implants of testosterone propionate (TP) induced PAs in 50-90% of rats respectively in an average of 11.5 months. The induction of PAs was prevented by early treatments of rats at risk with estradiol and less so with dihydrotestosterone (DHT). However, on a technical basis, the results were not significant. Treatments of MNU-inoculated rats with estradiol, with DHT, or by castration, at intermediate points in the projected latency time of tumor development, reduced significantly the incidences of PA development. Rats in which overt PAs had already developed in response to 12 months of exposure to implants of TP did not respond to treatment by estradiol, DHT, or castration. Thus there are early stage(s) in induced prostate tumorigenesis in L-W rats that are sensitive to modulating agents.

摘要

洛本德 - 威斯塔(L - W)大鼠在对自发性和诱发性转移性前列腺腺癌(PA)的易感性方面独具特点。单次静脉注射甲基亚硝基脲(MNU),在12个月内使20%的L - W大鼠发生PA。MNU与两到七个丙酸睾酮(TP)缓释植入剂联合使用,分别在平均11.5个月内使50 - 90%的大鼠发生PA。对有风险的大鼠早期用雌二醇治疗可预防PA的诱导,用二氢睾酮(DHT)治疗的预防效果稍差。然而,从技术层面讲,结果并不显著。在肿瘤发展的预计潜伏期中间点,用雌二醇、DHT或阉割处理MNU接种的大鼠,可显著降低PA发生的发生率。对因暴露于TP植入剂12个月而已经发生明显PA的大鼠,用雌二醇、DHT或阉割处理均无反应。因此,在L - W大鼠诱导性前列腺肿瘤发生过程中存在对调节因子敏感的早期阶段。

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