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类固醇诱导的实验啮齿动物泌尿生殖道变化及尿潴留

Steroid-induced urogenital tract changes and urine retention in laboratory rodents.

作者信息

Buhl A E, Yuan Y D, Cornette J C, Frielink R D, Knight K A, Ruppel P L, Kimball F A

出版信息

J Urol. 1985 Dec;134(6):1262-7. doi: 10.1016/s0022-5347(17)47708-1.

DOI:10.1016/s0022-5347(17)47708-1
PMID:4057428
Abstract

Since previous literature suggested that estrogen-treated male mice are models for human benign prostatic hypertrophy, a series of studies was designed to examine urine retention and urogenital tract changes in rodents given chronic estradiol-17 beta (E) and dihydrotestosterone (DHT) treatments. In Study 1, intact and castrate male mice received E, DHT or E plus DHT for four weeks via subcutaneous Silastic capsules. Bladder urine volume increased in the groups given E and this effect was not altered by castration, DHT or removal of E capsules two weeks before necropsy. Estrogen treatment also increased mortality. In Study 2, intact male, intact female, adrenalectomized (Adx) male and sham Adx male mice received 16 weeks of steroid treatments. Bladder urine volume increased in all E treated groups regardless of sex or Adx. Hydronephrosis, hydroureter and increased mortality were found in the E treated mice of both sexes. Estrogen induced epithelial changes and edema of the prostate, vas deferens and the utriculus prostaticus. In further studies male rats, hamsters and guinea pigs were given several different dosages of E but no evidence of urine retention or increased mortality was found. Taken together these studies suggest that E-induced urine retention is unique to mice. Although urine retention and hydronephrosis found in the mice were similar to those in humans with BPH, the lesion that results in the urine obstruction is not similar.

摘要

由于先前的文献表明,经雌激素处理的雄性小鼠可作为人类良性前列腺增生的模型,因此设计了一系列研究,以检查给予慢性17β-雌二醇(E)和双氢睾酮(DHT)处理的啮齿动物的尿潴留和泌尿生殖道变化。在研究1中,完整和去势的雄性小鼠通过皮下硅橡胶胶囊接受E、DHT或E加DHT处理四周。给予E的组膀胱尿量增加,且这种作用不会因去势、DHT或在尸检前两周取出E胶囊而改变。雌激素处理也增加了死亡率。在研究2中,完整雄性、完整雌性、肾上腺切除(Adx)雄性和假Adx雄性小鼠接受了16周的类固醇处理。无论性别或是否进行肾上腺切除,所有接受E处理的组膀胱尿量均增加。在接受E处理的两性小鼠中均发现肾积水、输尿管积水和死亡率增加。雌激素诱导前列腺、输精管和前列腺小囊的上皮变化和水肿。在进一步的研究中,给雄性大鼠、仓鼠和豚鼠给予几种不同剂量的E,但未发现尿潴留或死亡率增加的证据。综合这些研究表明,E诱导的尿潴留是小鼠特有的。尽管在小鼠中发现的尿潴留和肾积水与良性前列腺增生患者相似,但导致尿路梗阻的病变并不相似。

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Steroid-induced urogenital tract changes and urine retention in laboratory rodents.类固醇诱导的实验啮齿动物泌尿生殖道变化及尿潴留
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Urinary retention induced by estrogen injections in mice: an analytical model.雌激素注射诱导小鼠尿潴留:一种分析模型。
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Serum levels of follicle stimulating hormone, luteinizing hormone, prolactin, testosterone, 5 alpha-dihydrotestosterone, 5 alpha-androstane-3 alpha, 17 beta-diol, 5 alpha-androstane-3 beta, 17 beta-diol, and 17 beta-estradiol from male beagles with spontaneous or induced benign prostatic hyperplasia.来自患有自发性或诱发性良性前列腺增生的雄性比格犬的血清促卵泡激素、促黄体生成素、催乳素、睾酮、5α-二氢睾酮、5α-雄烷-3α,17β-二醇、5α-雄烷-3β,17β-二醇和17β-雌二醇水平。
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Dihydrotestosterone concentration of beagle prostatic tissue: effect of age and hyperplasia.比格犬前列腺组织的双氢睾酮浓度:年龄和增生的影响。
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Clinical Assessment of Urinary Tract Damage during Sustained-Release Estrogen Supplementation in Mice.小鼠持续释放雌激素补充过程中尿路损伤的临床评估
Comp Med. 2017 Feb 1;67(1):11-21.
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Environmental exposure, estrogen and two X chromosomes are required for disease development in an epigenetic model of lupus.环境暴露、雌激素和两个 X 染色体是疾病发展所必需的,这是狼疮的一种表观遗传模型。
J Autoimmun. 2012 May;38(2-3):J135-43. doi: 10.1016/j.jaut.2011.11.001. Epub 2011 Dec 3.
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Dose-dependent toxic effects of high-dose estrogen on renal and cardiac injury in surgically postmenopausal mice.大剂量雌激素对手术绝经后小鼠肾和心脏损伤的剂量依赖性毒性作用。
Life Sci. 2011 Jan 17;88(3-4):178-86. doi: 10.1016/j.lfs.2010.11.008. Epub 2010 Nov 11.