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子宫雌激素硫酸酯酶在介导硫酸雌酮的促子宫生长作用中可能比肝脏硫酸酯酶发挥更重要的作用。

Uterine estrogen sulfatase may play a more important role than the hepatic sulfatase in mediating the uterotropic action of estrone-3-sulfate.

作者信息

Zhu B T, Fu J H

机构信息

Department of Chemical Biology, College of Pharmacy, Rutgers, State University of New Jersey 08854-8020, USA.

出版信息

Endocrine. 1997 Oct;7(2):191-8. doi: 10.1007/BF02778141.

Abstract

The estrogenic activity of sulfonated estrogens results from the release of active estrogens via desulfonation (hydrolysis) catalyzed by estrogen sulfatase. In this study, the relative importance of uterine or hepatic estrone (E1)-3-sulfatase in mediating the uterotropic action of E1-3-sulfate is evaluated by comparing its hormonal potency in animals that have comparable uterine E1-3-sulfatase activity but markedly different hepatic enzyme activity. Liver microsomes from immature or adult female Sprague-Dawley rats contained 12- or 55-fold higher E1-3-sulfatase activity, respectively, than the liver microsomes from immature or adult female CD-1 mice. In contrast, uterine whole homogenates from immature female Sprague-Dawley rats contained approx twofold higher E1-3-sulfatase activity than was detected in the uterine whole homogenates from immature female CD-1 mice. It is estimated that the total E1-3-sulfatase activity in the liver of an immature female rat or mouse is approx 1080- or 260-fold higher, respectively, than the activity in the uterus. The ED50 values for the uterotropic effect of E1-3-sulfate and E1 in immature female CD-1 mice were 240 and 8 pmol/g body wt, respectively, and the corresponding ED50 values in immature female Sprague-Dawley rats were 840 and 60 pmol/g body wt, respectively. The difference in the ratios of the uterotropic ED50 for E1-3-sulfate over that for E1 in immature rats and mice (14 and 30, respectively) is 1.14-fold, which correlates very closely with their difference in the uterine E1-3-sulfatase activity (approx twofold), but not their difference in the hepatic sulfatase activity (approx 12-fold). The results of this study provide evidence suggesting that E1-3-sulfatase in the uterus (an estrogen target organ) may play a more important role than the hepatic sulfatase in mediating the uterotropic action of sulfonated estrogens.

摘要

磺酸化雌激素的雌激素活性源于雌激素硫酸酯酶催化的去磺酸化(水解)作用释放出活性雌激素。在本研究中,通过比较具有相当子宫E1-3-硫酸酯酶活性但肝酶活性明显不同的动物中E1-3-硫酸酯的激素效力,评估子宫或肝脏雌酮(E1)-3-硫酸酯酶在介导E1-3-硫酸盐的促子宫作用中的相对重要性。未成熟或成年雌性Sprague-Dawley大鼠的肝微粒体中E1-3-硫酸酯酶活性分别比未成熟或成年雌性CD-1小鼠的肝微粒体高12倍或55倍。相反,未成熟雌性Sprague-Dawley大鼠的子宫全匀浆中E1-3-硫酸酯酶活性比未成熟雌性CD-1小鼠子宫全匀浆中检测到的活性高约两倍。据估计,未成熟雌性大鼠或小鼠肝脏中总的E1-3-硫酸酯酶活性分别比子宫中的活性高约1080倍或260倍。未成熟雌性CD-1小鼠中E1-3-硫酸盐和E1促子宫作用的半数有效剂量(ED50)值分别为240和8 pmol/g体重,未成熟雌性Sprague-Dawley大鼠中相应的ED50值分别为840和60 pmol/g体重。未成熟大鼠和小鼠中E1-3-硫酸盐促子宫ED50与E1促子宫ED50的比值差异(分别为14和30)为1.14倍,这与其子宫E1-3-硫酸酯酶活性差异(约两倍)密切相关,但与它们肝脏硫酸酯酶活性差异(约12倍)无关。本研究结果提供了证据,表明子宫(雌激素靶器官)中的E1-3-硫酸酯酶在介导磺酸化雌激素的促子宫作用中可能比肝脏硫酸酯酶发挥更重要的作用。

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