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低水平表达人生长激素的转基因大鼠肝脏细胞色素P450同工酶组成的特征分析

Characterization of hepatic cytochrome P450 isozyme composition in the transgenic rat expressing low level human growth hormone.

作者信息

Takahashi J, Furuhata Y, Ikeda A, Takahashi M, Iwata H, Kazusaka A, Fujita S

机构信息

Department of Environmental Veterinary Sciences, Graduate School of Veterinary Medicine, Hokkaido University, Sapporo, Japan.

出版信息

Xenobiotica. 1999 Dec;29(12):1203-12. doi: 10.1080/004982599237886.

Abstract
  1. The present authors have previously developed a transgenic rat carrying a chimeric gene of the mouse whey acidic protein promoter and the structural portion of human growth hormone (GH) gene. Among this (hGH-TG) rat, a line (low GH rat) missing a male-specific pulsatile GH secretary pattern due to suppression of endogenous GH secretion and having a continuous low GH (hGH and rat GH) level in the peripheral circulation was identified. The latter rat was also characterized as having severe obesity with age. This strain (low Gh rat) was used to correlate the sex-specific secretory pattern of GH with the sex-specific expression of cytochrome P450 (CYP) in rat. 2. Comparisons were made between the low GH rat and the non-transgenic rat as to the expression of liver microsomal CYP isozymes. The following enzyme activities were assessed: testosterone (T) hydroxylation and oxidation; ethoxyresorufin O-dealkylation (EROD); bunitrolol (BTL) 4-hydroxylation and T5 alpha-reduction. Protein expression of CYP1A, CYP2C11, CYP2D, CYP2E1, CYP3A2 and CYP4A1 were also assessed by Western blot analysis. 3. Enzyme activities and protein expression of CYP2C11 (T16 alpha and 2alpha-hydroxylase and 17-oxidase activities) and CYP3A2 (T6beta and 2beta-hydroxylase activities) levels, which are known to be higher in the male than in the female rat, were significantly lower in the adult male low GH rat than in the control male rat. In contrast, CYP2A1 (T7 alpha-hydroxylase) and T5-alpha-reductase activities, which are known to be specifically elevated in the female, were significantly higher in the adult male low GH rat than in the control male rat. Thus, the loss of male-specific secretory pattern of GH results in feminization of the pattern of expression of CYP and T5 alpha-reductase activity in the liver. 4. In contrast to other GH-deficient models so far studied, an increase in CYP4A1 and a decrease in CYP2E1 protein expression were observed in the low GH rat. These trends are consistent with the characteristic phenotype of obesity in the transgenic rat because CYP4A1 and CYP2E1 enhance fatty acid excretion and glyconeogenesis from fatty acids respectively.
摘要
  1. 本研究作者先前培育出一种转基因大鼠,其携带小鼠乳清酸性蛋白启动子与人生长激素(GH)基因结构部分的嵌合基因。在这种(hGH-TG)大鼠中,鉴定出一个品系(低GH大鼠),由于内源性GH分泌受抑制,其缺乏雄性特异性的脉冲式GH分泌模式,外周循环中GH(hGH和大鼠GH)水平持续较低。后一种大鼠还表现出随年龄增长而严重肥胖的特征。该品系(低Gh大鼠)被用于研究GH的性别特异性分泌模式与大鼠细胞色素P450(CYP)的性别特异性表达之间的关系。2. 对低GH大鼠和非转基因大鼠肝脏微粒体CYP同工酶的表达进行了比较。评估了以下酶活性:睾酮(T)羟基化和氧化;乙氧异羟肟酸O-脱烷基化(EROD);布尼洛尔(BTL)4-羟基化和T5α-还原。还通过蛋白质印迹分析评估了CYP1A、CYP2C11、CYP2D、CYP2E1、CYP3A2和CYP4A1的蛋白质表达。3. CYP2C11(T16α和2α-羟化酶及17-氧化酶活性)和CYP3A2(T6β和2β-羟化酶活性)的酶活性和蛋白质表达水平,已知在雄性大鼠中高于雌性大鼠,在成年雄性低GH大鼠中显著低于对照雄性大鼠。相反,已知在雌性中特异性升高的CYP2A1(T7α-羟化酶)和T5-α-还原酶活性,在成年雄性低GH大鼠中显著高于对照雄性大鼠。因此,GH雄性特异性分泌模式的丧失导致肝脏中CYP表达模式和T5α-还原酶活性的女性化。4. 与迄今为止研究的其他GH缺乏模型不同,在低GH大鼠中观察到CYP4A1增加和CYP2E1蛋白质表达减少。这些趋势与转基因大鼠肥胖的特征表型一致,因为CYP4A1和CYP2E1分别增强脂肪酸排泄和脂肪酸糖异生。

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