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人类肾上腺在发育和衰老过程中脱氢表雄酮及硫酸脱氢表雄酮的生成

Dehydroepiandrosterone and dehydroepiandrosterone sulfate production in the human adrenal during development and aging.

作者信息

Parker C R

机构信息

Department of Obstetrics and Gynecology, University of Alabama at Birmingham 35233-7333, USA.

出版信息

Steroids. 1999 Sep;64(9):640-7. doi: 10.1016/s0039-128x(99)00046-x.

Abstract

Dehydroepiandrosterone (DHEA) is produced in prodigious quantities by the human adrenal, principally as the 3-sulfoconjugate DHEA sulfate (DS) during intrauterine life. The fetal zone and neocortex cells of the fetal adrenal express large amounts of DHEA sulfotransferase and minimal amounts, at least until very near the end of gestation, of 3beta-hydroxysteroid dehydrogenase. This pattern of enzyme expression favors substantial secretion of DHEA/DS with minimal cortisol produced; the DHEA/DS serves as the major precursor for placental estrogen formation in human pregnancy. Aside from adrenocorticotropin, other physiologic regulators of growth and steroidogenesis in the fetal adrenal have been postulated to exist, but have yet to be identified. Whereas intrauterine stressors may activate adrenal cortisol secretion, the fetal adrenal responds to many pregnancy conditions by suppressing DHEA/DS formation. After birth, the human adrenal undergoes reorganization whereby the large, inner fetal zone regresses, and DHEA/DS production is diminished. Just prior to gonadal maturation, the human adrenal undergoes morphologic and functional changes (adrenarche) that give rise to a prominent zona reticularis that is characterized by the presence of DHEA sulfotransferase, the absence of 3beta-hydroxysteroid dehydrogenase, and an enhancement of DHEA/DS production. The adrenal of the adult responds to stress in many instances like that of the fetus: increased cortisol secretion and diminished DHEA/DS secretion. The mechanisms for this divergence in the adrenocortical pathway is unknown. With aging, there is suppression of DHEA/DS secretion, possibly as the consequence of an involution of the zona reticularis, but corticosteroid production continues unabated.

摘要

脱氢表雄酮(DHEA)由人类肾上腺大量分泌,在子宫内主要以3 - 硫酸共轭脱氢表雄酮(DS)的形式存在。胎儿肾上腺的胎儿带和新皮质细胞表达大量的DHEA硫酸转移酶,而3β - 羟基类固醇脱氢酶的表达量极少,至少在妊娠末期之前都是如此。这种酶表达模式有利于大量分泌DHEA/DS,而产生的皮质醇极少;在人类妊娠中,DHEA/DS是胎盘雌激素形成的主要前体。除促肾上腺皮质激素外,胎儿肾上腺生长和类固醇生成的其他生理调节因子已被推测存在,但尚未被鉴定出来。虽然子宫内应激源可能会激活肾上腺皮质醇分泌,但胎儿肾上腺对许多妊娠情况的反应是抑制DHEA/DS的形成。出生后,人类肾上腺会进行重组,大的内部胎儿带退化,DHEA/DS的产生减少。就在性腺成熟之前,人类肾上腺会发生形态和功能变化(肾上腺初现),形成一个突出的网状带,其特征是存在DHEA硫酸转移酶,缺乏3β - 羟基类固醇脱氢酶,且DHEA/DS的产生增加。在许多情况下,成人肾上腺对压力的反应与胎儿相似:皮质醇分泌增加,DHEA/DS分泌减少。肾上腺皮质途径中这种差异的机制尚不清楚。随着年龄增长,DHEA/DS分泌受到抑制,这可能是网状带退化的结果,但皮质类固醇的产生仍未减弱。

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