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睾酮在人前列腺和精囊中的代谢。

Metabolism of testosterone in the human prostate and seminal vesicles.

作者信息

Kjoseland O, Tveter K J, Attramadal A, Hansson V, Haugen H N, Mathisen W

出版信息

Scand J Urol Nephrol. 1977;11(1):1-6. doi: 10.3109/00365597709179684.

Abstract

Tissue from the normal, hyperplastic and the cancerous human prostate as well as tissue from the human seminal vesicles are capable of metabolizing testosterone in vitro. By incubating minced tissue with 3H-testosterone for 2 hours at 37 degrees C the following radioactive metabolites were identified: testosterone (17 beta-hydroxyl-4-androsten-3-one), androstenedione (4-androstene-3,17-dione), androstanedione (5alpha-androstane-3,17-dione), 5alpha-dihydrostestosterone (17 beta-hydroxy-5alpha-androstane-3-one, DHT), 3alpha-androstanediol (5alpha-androstane-3alpha,17beta-diol), 3beta-androstanediol (5alpha-androstane-3beta-17beta-diol) and androsterone (3alpha-hydroxy-5alpha-androstane-17-one). When normal human prostatic tissue was incubated with 3H-testosterone approximately 40% of the hormone was metabolized and 30-35% of the metabolites were identified as DHT. There were apparently no differences in testosterone metabolism between the dorsal and lateral prostatic lobes. A much lower conversion of 3H-testosterone was observed in the seminal vesicles (24%). The same metabolites were formed by prostatic carcinoma tissue, although distinctive quantitative differences from the normal prostate were observed. Thus, only 23% of the testosterone was metabolized by cancerous tissue of which 15% was present as DHT. The formation of 17-keto metabolites and androstanediols in the prostatic carcinoma tissue was approximately the same as in the normal prostatic tissue. The most extensive metabolism of testosterone was found by incubation of tissue from benign nodular prostatic hyperplasia. About 65% of the testosterone was metabolized, and 40% of the metabolites were identified as DHT. Hyperplastic prostatic tissue also showed a significantly higher formation of 5alpha-androstanedoils and the other tissues examined. The high formation of DHT and 5alpha-androstanediols in benign nodular prostatic hyperplasia in comparison with normal and cancerous prostatic tissue and seminal vesicle tissue might indicate that these metabolites should be studied more closely as possible aetiological factors for prostatic hyperplasia. The very low metabolism of testosterone in prostatic carcinoma tissue should be examined further in relation to tumour differentiation and clinical effect of endocrine therapy.

摘要

来自正常、增生及癌性人前列腺的组织以及来自人精囊的组织在体外均能够代谢睾酮。通过在37℃下将切碎的组织与³H - 睾酮孵育2小时,鉴定出了以下放射性代谢产物:睾酮(17β - 羟基 - 4 - 雄烯 - 3 - 酮)、雄烯二酮(4 - 雄烯 - 3,17 - 二酮)、雄烷二酮(5α - 雄烷 - 3,17 - 二酮)、5α - 双氢睾酮(17β - 羟基 - 5α - 雄烷 - 3 - 酮,DHT)、3α - 雄烷二醇(5α - 雄烷 - 3α,17β - 二醇)、3β - 雄烷二醇(5α - 雄烷 - 3β - 17β - 二醇)和雄酮(3α - 羟基 - 5α - 雄烷 - 17 - 酮)。当将正常人前列腺组织与³H - 睾酮孵育时,约40%的激素被代谢,且30 - 35%的代谢产物被鉴定为DHT。前列腺背叶和侧叶之间的睾酮代谢显然没有差异。在精囊中观察到³H - 睾酮的转化率要低得多(24%)。前列腺癌组织也形成相同的代谢产物,尽管与正常前列腺组织存在明显的定量差异。因此,癌组织仅代谢23%的睾酮,其中15%以DHT形式存在。前列腺癌组织中17 - 酮代谢产物和雄烷二醇的形成与正常前列腺组织大致相同。通过对良性结节性前列腺增生组织的孵育发现睾酮的代谢最为广泛。约65%的睾酮被代谢,且40%的代谢产物被鉴定为DHT。增生性前列腺组织与正常和癌性前列腺组织以及精囊组织相比,5α - 雄烷二醇的形成也显著更高。与正常和癌性前列腺组织以及精囊组织相比,良性结节性前列腺增生中DHT和5α - 雄烷二醇的高形成可能表明这些代谢产物作为前列腺增生可能的病因学因素应得到更深入的研究。前列腺癌组织中睾酮的极低代谢应结合肿瘤分化和内分泌治疗的临床效果进一步研究。

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