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衰老比格犬中二氢睾酮代谢的变化与良性前列腺增生的发展

Changes in dihydrotestosterone metabolism and the development of benign prostatic hyperplasia in the aging beagle.

作者信息

Isaacs J T

出版信息

J Steroid Biochem. 1983 Jun;18(6):749-57. doi: 10.1016/0022-4731(83)90255-8.

DOI:10.1016/0022-4731(83)90255-8
PMID:6191128
Abstract

Previous studies have demonstrated that the 2-3--fold abnormal elevation in prostatic dihydrotestosterone (DHT) content characteristically associated with canine benign prostatic hyperplasia (BPH) is due to a shift in the overall balance in the complex metabolism of DHT in the gland itself [1, 2]. Since the incidence of canine BPH increases with host age [3], the question arises as to whether the characteristic shift in DHT metabolism is associated with the general process of aging or with the specific development of BPH. To resolve this issue, the activities of prostatic androgen metabolism were quantitatively assayed in prostatic tissue from a large series of age-matched normal and BPH dogs ranging in age from 0.7-9.0 years. These analyses revealed that, regardless of the age of the host, there is a consistent statistical increase in several of the activities which produce DHT (i.e. 5 alpha-reductase, 3 alpha-HSOR oxidase, and 17 beta-HSOR reductase) without a concomitant increase in any of the activities which remove this steroid in BPH as compared to age-matched normal prostatic tissue. These results suggest that in canine BPH tissue the characteristic changes in DHT metabolism which increase the tissue's ability for net formation of DHT are specifically associated with the development of BPH itself and not due simply to the general process of aging per se.

摘要

先前的研究表明,犬良性前列腺增生(BPH)特征性地伴有前列腺二氢睾酮(DHT)含量2 - 3倍的异常升高,这是由于腺体自身DHT复杂代谢的整体平衡发生了改变[1, 2]。由于犬BPH的发病率随宿主年龄增加而上升[3],因此出现了这样一个问题,即DHT代谢的特征性改变是与衰老的一般过程相关,还是与BPH的特定发展相关。为了解决这个问题,对大量年龄在0.7 - 9.0岁的年龄匹配的正常犬和患BPH犬的前列腺组织中前列腺雄激素代谢活性进行了定量测定。这些分析表明,无论宿主年龄如何,与年龄匹配的正常前列腺组织相比,在BPH中,几种产生DHT的活性(即5α - 还原酶、3α - HSOR氧化酶和17β - HSOR还原酶)在统计学上持续增加,而消除这种类固醇的任何活性均未随之增加。这些结果表明,在犬BPH组织中,DHT代谢的特征性变化增加了组织净生成DHT的能力,这与BPH自身的发展具体相关,而不仅仅是由于衰老本身的一般过程。

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