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大鼠肝脏糖皮质激素受体与钨酸钠的相互作用。

Interaction of rat liver glucocorticoid receptor with sodium tungstate.

作者信息

Murakami N, Healy S P, Moudgil V K

出版信息

Biochem J. 1982 Jun 15;204(3):777-86. doi: 10.1042/bj2040777.

Abstract

Effects of sodium tungstate on various properties of rat liver glucocorticoid receptor were examined at pH7 and pH 8. At pH 7, [3H]triamcinolone acetonide binding in rat liver cytosol preparations was completely blocked in the presence of 10--20 mM-sodium tungstate at 4 degrees C, whereas at 37 degrees C a 30 min incubation of cytosol receptor preparation with 1 mM-sodium tungstate reduced the loss of unoccupied receptor by 50%. At pH 8.0, tungstate presence during the 37 degrees C incubation maintained the steroid-binding capacity of unoccupied glucocorticoid receptor at control (4 degrees C) levels. In addition, heat-activation of cytosolic glucocorticoid-receptor complex was blocked by 1 mM- and 10 mM-sodium tungstate at pH 7 and pH 8 respectively. The DNA-cellulose binding by activated receptor was also inhibited completely and irreversibly by 5 mM-tungstate at pH 7, whereas at pH 8 no significant effect was observed with up to 20 mM-tungstate. The entire DNA-cellulose-bound glucocorticoid-receptor complex from control samples could be extracted by incubation with 1 mM- and 20 mM-tungstate at pH 7 and pH 8 respectively, and appeared to sediment as a 4.3--4.6 S molecule, both in 0.01 M- and 0.3 M-KCl-containing sucrose gradients. Tungstate effects are, therefore, pH-dependent and appear to involve an interaction with both the non-activated and the activated forms of the glucocorticoid receptor.

摘要

在pH7和pH8条件下研究了钨酸钠对大鼠肝脏糖皮质激素受体各种特性的影响。在pH7时,4℃下,10-20mM钨酸钠存在时,大鼠肝脏胞质溶胶制剂中[3H]曲安奈德结合被完全阻断,而在37℃时,胞质溶胶受体制剂与1mM钨酸钠孵育30分钟可使未占据受体的损失减少50%。在pH8.0时,37℃孵育期间存在钨酸盐可使未占据糖皮质激素受体的类固醇结合能力维持在对照(4℃)水平。此外,在pH7和pH8时,1mM和10mM钨酸钠分别阻断了胞质糖皮质激素受体复合物的热激活。在pH7时,5mM钨酸盐也完全不可逆地抑制了活化受体与DNA纤维素的结合,而在pH8时,高达20mM钨酸盐未观察到显著影响。对照样品中与DNA纤维素结合的整个糖皮质激素受体复合物分别在pH7和pH8时与1mM和20mM钨酸盐孵育可被提取,并且在含0.01M和0.3M KCl的蔗糖梯度中似乎以4.3-4.6S分子形式沉降。因此,钨酸盐的作用是pH依赖性的,并且似乎涉及与糖皮质激素受体的非活化和活化形式的相互作用。

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