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脱氢表雄酮与外周靶组织中雄激素和雌激素的内分泌形成:其在衰老过程中的作用。

DHEA and the intracrine formation of androgens and estrogens in peripheral target tissues: its role during aging.

作者信息

Labrie F, Bélanger A, Luu-The V, Labrie C, Simard J, Cusan L, Gomez J L, Candas B

机构信息

Laboratory of Molecular Endocrinology, CHUL (Le Centre Hospitalier de l'Université Laval) Research Center, Québec, Canada.

出版信息

Steroids. 1998 May-Jun;63(5-6):322-8. doi: 10.1016/s0039-128x(98)00007-5.

Abstract

Human and some other primates are unique since their adrenals secrete large amounts of dehydroepiandrosterone (DHEA) and its sulfate (DHEA-S), which are converted into androstenedione (4-dione) and then into potent androgens and estrogens in peripheral tissues, therefore providing autonomous intracrine control to target tissues that can adjust the formation and metabolism of active sex steroids according to local requirements. Knowledge in this area has recently made rapid progress with the elucidation of the structure of most of the tissue-specific cDNAs and genes that encode the steroidogenic enzymes responsible for the transformation of these inactive precursor steroids into androgens and/or estrogens. It is estimated that 30 to 50% of total androgens in men are synthesized in peripheral intracrine tissues from inactive adrenal precursors while, in women, peripheral estrogen formation is even more important, the best estimate being 75% before menopause and 100% after menopause. The marked reduction in the formation of DHEA-S by the adrenals during aging, especially before the age of 50 years, results in a dramatic fall in the formation of active sex steroids in peripheral target tissues, a situation which is thought to be associated with a long series of age-related decreases such as insulin resistance, obesity, osteoporosis, cardiovascular diseases, loss of muscle mass, cancer and other diseases. We have demonstrated for the first time a series of medically important beneficial effects of DHEA administered for 12 months to post-menopausal women. Most interestingly, the bone mineral density significantly increased. This relatively rapid change was associated with an increase in plasma osteocalcin, a marker of bone formation, while a decrease in bone resorption reflected by a decrease in urinary hydroxyproline excretion was observed in parallel. In addition, the estrogenic stimulation of vaginal cytology in the absence of any sign of stimulatory effect on the endometrium is also of potentially major interest for the prevention and management of menopause. Furthermore, the inhibitory effect of DHEA on the growth of human breast cancer xenografts in vivo in nude mice supports the beneficial use of DHEA as hormone replacement therapy in women.

摘要

人类和其他一些灵长类动物很独特,因为它们的肾上腺会分泌大量脱氢表雄酮(DHEA)及其硫酸盐(DHEA-S),这些物质在外周组织中会转化为雄烯二酮(4-二酮),然后再转化为强效雄激素和雌激素,从而为靶组织提供自主性内分泌控制,使其能够根据局部需求调节活性甾体激素的生成和代谢。随着大多数组织特异性cDNA和基因结构的阐明,该领域的知识最近取得了快速进展,这些cDNA和基因编码负责将这些无活性前体甾体激素转化为雄激素和/或雌激素的甾体生成酶。据估计,男性体内30%至50%的雄激素是由外周内分泌组织从无活性的肾上腺前体合成的,而在女性中,外周雌激素的生成更为重要,最佳估计是绝经前为75%,绝经后为100%。随着年龄增长,尤其是在50岁之前,肾上腺分泌DHEA-S的能力显著下降,导致外周靶组织中活性甾体激素的生成急剧减少,这种情况被认为与一系列与年龄相关的衰退有关,如胰岛素抵抗、肥胖、骨质疏松、心血管疾病、肌肉量减少、癌症和其他疾病。我们首次证明了给绝经后女性服用DHEA 12个月具有一系列重要的医学有益效果。最有趣的是,骨矿物质密度显著增加。这种相对快速的变化与血浆骨钙素增加有关,骨钙素是骨形成的标志物,同时观察到尿羟脯氨酸排泄减少反映的骨吸收减少与之平行。此外,在对子宫内膜无任何刺激作用迹象的情况下,DHEA对阴道细胞学的雌激素刺激作用对于绝经的预防和管理也可能具有重要意义。此外,DHEA对裸鼠体内人乳腺癌异种移植瘤生长的抑制作用支持了DHEA作为女性激素替代疗法的有益应用。

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