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下丘脑 - 垂体对大鼠肝脏细胞色素P - 450(15)β载脂蛋白水平的调节

Hypothalamo-pituitary regulation of cytochrome P-450(15) beta apoprotein levels in rat liver.

作者信息

MacGeoch C, Morgan E T, Gustafsson J A

出版信息

Endocrinology. 1985 Nov;117(5):2085-92. doi: 10.1210/endo-117-5-2085.

Abstract

The regulation of the sexually differentiated steroid sulfate 15 beta-hydroxylase, cytochrome P-450(15) beta of female rat liver has been investigated. Specific antibodies raised to isozyme P-450(15) beta were used with the Western blot technique to quantitate the specific levels of P-450(15) beta in liver microsomes. The method demonstrated that the levels of the protein are about 16-fold higher in female than in male microsomes and also showed that the specific microsomal content of P-450(15) beta is controlled by GH. Hypophysectomy of female animals resulted in a decrease of P-450(15) beta to male levels. Continuous infusion of human GH, mimicking the female pattern of GH secretion in intact male animals, caused an elevation of the P-450(15) beta level to that of the female. The same dose of human GH in hypophysectomized male or female animals raised the P-450(15) beta level 8-fold or 50% of that seen in normal females. Infusion of ovine PRL to intact male rats had no effect on P-450(15) beta levels, whereas infusion of rat GH caused a 4-fold increase. Thus, the regulation of P-450(15) beta by GH is mainly associated with the somatogenic properties of the hormone. Furthermore, sc injection of rat GH every 12 h, mimicking the male pattern of GH secretion, had no effect on P-450(15) beta levels, demonstrating the importance of the GH secretory pattern in regulation of the specific protein levels. Postpubertal castration of male animals did not influence the microsomal P-450(15) beta content, whereas neonatal castration led to a feminization of the P-450(15) beta content in the adult male rat. Administration of estradiol valerate to male animals caused complete feminization of P-450(15) beta levels, whereas administration of androgen to female animals caused a decrease to male levels. Before 21 days of age, the P-450(15) beta level was slightly higher in male than in female rats. At 35 days, however, the P-450(15) beta level in female rats had increased almost 100-fold, whereas the levels in males increased only slightly. These changes are concomitant with the development of the sexual differentiation of the GH secretory pattern, supporting the role of GH in P-450(15) beta regulation. In conclusion, isozyme P-450(15) beta is a GH-regulated enzyme specific for female rats. The low level of the protein in males is probably explained by neonatal androgenic programming of the GH secretory pattern.

摘要

对雌性大鼠肝脏中具有性别差异的硫酸类固醇15β-羟化酶(细胞色素P-450(15)β)的调节进行了研究。用针对同工酶P-450(15)β产生的特异性抗体与蛋白质印迹技术相结合,来定量肝脏微粒体中P-450(15)β的特定水平。该方法表明,雌性微粒体中该蛋白质的水平比雄性微粒体中的高约16倍,并且还表明P-450(15)β的特定微粒体含量受生长激素(GH)控制。对雌性动物进行垂体切除导致P-450(15)β水平降至雄性水平。在完整的雄性动物中持续输注人GH,模拟雌性GH分泌模式,可使P-450(15)β水平升高至雌性水平。在垂体切除的雄性或雌性动物中给予相同剂量的人GH,可使P-450(15)β水平分别升高8倍或达到正常雌性动物的50%。向完整的雄性大鼠输注绵羊催乳素(PRL)对P-450(15)β水平没有影响,而输注大鼠GH则使其增加4倍。因此,GH对P-450(15)β的调节主要与该激素的促生长特性有关。此外,每12小时皮下注射大鼠GH,模拟雄性GH分泌模式,对P-450(15)β水平没有影响,这表明GH分泌模式在调节特定蛋白质水平方面的重要性。雄性动物青春期后去势不影响微粒体P-450(15)β含量,而新生期去势则导致成年雄性大鼠P-450(15)β含量出现雌性化。给雄性动物施用戊酸雌二醇会使P-450(15)β水平完全雌性化,而给雌性动物施用雄激素则会使其降至雄性水平。在21日龄之前,雄性大鼠的P-450(15)β水平略高于雌性大鼠。然而,在35日龄时,雌性大鼠的P-450(15)β水平几乎增加了100倍,而雄性大鼠的水平仅略有增加。这些变化与GH分泌模式的性别分化发育同步,支持了GH在P-450(图15)β调节中的作用。总之,同工酶P-450(15)β是一种受GH调节的、对雌性大鼠具有特异性的酶。雄性中该蛋白质的低水平可能是由于GH分泌模式的新生期雄激素编程所致。

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