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雄激素对大鼠前列腺、精囊和肾脏中视黄酸受体信使核糖核酸的调节作用。

Androgen modulation of the messenger ribonucleic acid of retinoic acid receptors in the prostate, seminal vesicles, and kidney in the rat.

作者信息

Huang H F, Li M T, Von Hagen S, Zhang Y F, Irwin R J

机构信息

Department of Surgery, University of Medicine and Dentistry of New Jersey Medical School, Newark 07103, USA.

出版信息

Endocrinology. 1997 Feb;138(2):553-9. doi: 10.1210/endo.138.2.4945.

Abstract

Previously, we reported that the steady state level of messenger RNA (mRNA) transcripts of retinoic acid receptors (RAR) alpha and gamma in the testes of 20-day-old rats can be modulated by exogenous testosterone. These results suggest that androgen regulation of Sertoli cell functions may involve biochemical events mediated by RAR genes. In this study, we examined the effects of castration and testosterone replacement on the steady state level of mRNA transcripts for RAR alpha and gamma in the prostate, seminal vesicles, and kidney of the rat. Northern blot analysis revealed that in intact adult rats, the relative steady state levels of the 3.4- and 2.7-kilobase (kb) mRNA transcripts for RAR alpha and the 3.4-kb transcript for RAR gamma in the prostate were at least 20-fold higher than those in the seminal vesicles and kidney. The relatively high abundance of RAR mRNA transcripts in the prostate suggests the physiological importance of RAR-mediated processes in this organ. Castration resulted in an increase in the level of RAR mRNA transcripts in the prostate and seminal vesicles, reaching a maximum of 2- to 4-fold in the prostate and 15- to 23-fold in the seminal vesicles within 6 days. On the other hand, the levels of mRNA transcripts of RAR alpha and -gamma in the kidney were reduced by 40-50% 1 day after castration. The effects of castration on RAR mRNA levels in all three organs were prevented by implantation of 3-cm testosterone capsules at the time of castration, a regimen that provides physiological levels of serum testosterone. In a subsequent experiment, adult male rats were given a single sc injection of 2 mg testosterone 3 days after castration. This treatment resulted in an acute suppression of the level of RAR mRNA transcripts in all three organs within 30 min. Thereafter, the levels of RAR alpha and -gamma mRNA transcripts in the prostate continued to decrease, whereas those in the seminal vesicles returned to the castrated levels within 6 h. On the other hand, RAR mRNA levels in the kidney rebounded by 1 h and remained at the level found in the untreated castrated rats. These results demonstrate that the steady state level of mRNA transcripts for RAR alpha and -gamma in the prostate, seminal vesicles, and kidney can be modulated by testosterone in organ-specific manners, thus suggesting that the RAR-mediated processes may be involved in the effects of androgen in these organs. Furthermore, the relatively low increment in prostatic RAR mRNA levels after castration compared to that in the seminal vesicles demonstrates a difference in androgen responses between these two organs. This difference could dictate the efficacy of the effects of androgen on cellular function and may contribute to the disparate vulnerabilities to androgen-related uncontrolled cell proliferation and/or malignancy in the prostate and seminal vesicles.

摘要

此前,我们报道过,20日龄大鼠睾丸中视黄酸受体(RAR)α和γ的信使核糖核酸(mRNA)转录本的稳态水平可受外源性睾酮调节。这些结果表明,雄激素对支持细胞功能的调节可能涉及由RAR基因介导的生化事件。在本研究中,我们检测了去势及睾酮替代对大鼠前列腺、精囊和肾脏中RARα和γ的mRNA转录本稳态水平的影响。Northern印迹分析显示,在成年未阉割大鼠中,前列腺中RARα的3.4千碱基(kb)和2.7 kb mRNA转录本以及RARγ的3.4 kb转录本的相对稳态水平比精囊和肾脏中的至少高20倍。前列腺中RAR mRNA转录本相对丰度较高,表明RAR介导的过程在该器官中具有生理重要性。去势导致前列腺和精囊中RAR mRNA转录本水平升高,在6天内前列腺中最高升高2至4倍,精囊中升高15至23倍。另一方面,去势1天后,肾脏中RARα和γ的mRNA转录本水平降低40 - 50%。在去势时植入3厘米睾酮胶囊(该方案可提供生理水平的血清睾酮)可防止去势对所有三个器官中RAR mRNA水平的影响。在随后的实验中,成年雄性大鼠在去势3天后单次皮下注射2毫克睾酮。该处理导致所有三个器官中RAR mRNA转录本水平在30分钟内急性下降。此后,前列腺中RARα和γ的mRNA转录本水平继续下降,而精囊中这些转录本水平在6小时内恢复到去势后的水平。另一方面,肾脏中RAR mRNA水平在1小时后反弹,并维持在未处理去势大鼠中的水平。这些结果表明,睾酮可通过器官特异性方式调节前列腺、精囊和肾脏中RARα和γ的mRNA转录本稳态水平,因此提示RAR介导的过程可能参与雄激素在这些器官中的作用。此外,与精囊相比,去势后前列腺中RAR mRNA水平升高幅度相对较小,表明这两个器官在雄激素反应方面存在差异。这种差异可能决定雄激素对细胞功能影响的效力,并可能导致前列腺和精囊在与雄激素相关的不受控制的细胞增殖和/或恶性肿瘤方面的不同易感性。

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