Waxman D J, Ram P A, Pampori N A, Shapiro B H
Department of Biology, Boston University, Massachusetts 02215, USA.
Mol Pharmacol. 1995 Nov;48(5):790-7.
Growth hormone (GH) secretory patterns regulate the expression of several sex-dependent liver cytochrome P450 (CYP) genes. Studies using the hypophysectomized rat model have established that the intermittent plasma GH secretory pattern associated with adult male rats markedly stimulates liver expression of the male-specific CYP 2C11, a testosterone 2 alpha- and 16 alpha-hydroxylase, but is not required for expression of other male-specific liver enzymes, including CYP 2A2, a testosterone 15 alpha-hydroxylase, and CYP 3A2, a testosterone 6 beta-hydroxylase. In the present study, the effects of intermittent GH treatment on liver CYP expression were studied in adult rats rendered GH deficient by neonatal administration of monosodium glutamate (MSG), which depletes circulating adult GH without the global loss of other pituitary-dependent hormones that is associated with hypophysectomy. Restoration of the normal masculine circulating GH profile of six daily pulses (180-225 ng GH/ml/peak) in MSG-treated male rats by the use of an external pumping apparatus led to a substantial (30-50%) restoration of normal male levels of CYP 2A2 and CYP 3A2 activity, protein, and mRNA. GH pulsation at the nonphysiological frequencies of two or four times per day was less effective unless given at a dose that resulted in supraphysiological plasma GH levels. Although intermittent GH treatment can induce male-specific P450 expression in hypophysectomized female rats, the same hormone treatment did not stimulate CYP 2A2 or CYP 3A2 expression in MSG-treated female rats. Liver GH receptor mRNA levels at adulthood were not significantly altered by neonatal MSG treatment, suggesting that the unresponsiveness of MSG-treated females and the previously reported low responsiveness of MSG-treated males to GH-induced CYP 2C11 expression are not due to the absence of GH receptor. Moreover, normal liver IGF-1 mRNA levels were expressed in the MSG-treated female rats, suggesting that the liver GH receptor is functional in these animals. The present findings establish that the adult male-specific enzymes CYP 2A2 and CYP 3A2 can be positively regulated by intermittent GH pulsation despite their GH-independent expression in hypophysectomized rats. Moreover, neonatal MSG treatment, particularly in female rats, may lead to the loss of factors other than GH that are required for full expression of the pulsatile GH-stimulated CYP 2A2, 3A2, and 2C11 genes.
生长激素(GH)的分泌模式调节几种性别依赖性肝脏细胞色素P450(CYP)基因的表达。使用垂体切除大鼠模型的研究表明,与成年雄性大鼠相关的间歇性血浆GH分泌模式显著刺激雄性特异性CYP 2C11(一种睾酮2α-和16α-羟化酶)的肝脏表达,但对于其他雄性特异性肝脏酶的表达并非必需,包括睾酮15α-羟化酶CYP 2A2和睾酮6β-羟化酶CYP 3A2。在本研究中,通过新生期给予谷氨酸单钠(MSG)使成年大鼠GH缺乏,研究了间歇性GH治疗对肝脏CYP表达的影响,MSG可消耗循环中的成年GH,而不会像垂体切除那样导致其他垂体依赖性激素的整体丧失。通过使用外部泵装置恢复MSG处理的雄性大鼠正常的每日六次脉冲(180 - 225 ng GH/ml/峰值)的男性化循环GH谱,导致CYP 2A2和CYP 3A2活性、蛋白质和mRNA的正常男性水平大幅(30 - 50%)恢复。每天两次或四次的非生理频率的GH脉冲效果较差,除非给予导致超生理血浆GH水平的剂量。虽然间歇性GH治疗可诱导垂体切除的雌性大鼠中雄性特异性P450表达,但相同的激素治疗并未刺激MSG处理的雌性大鼠中CYP 2A2或CYP 3A2的表达。新生期MSG处理并未显著改变成年期肝脏GH受体mRNA水平,这表明MSG处理的雌性大鼠无反应以及先前报道的MSG处理的雄性大鼠对GH诱导的CYP 2C11表达反应低下并非由于缺乏GH受体。此外,MSG处理的雌性大鼠中正常表达肝脏IGF - 1 mRNA水平,表明肝脏GH受体在这些动物中具有功能。本研究结果表明,成年雄性特异性酶CYP 2A2和CYP 3A2可受到间歇性GH脉冲的正向调节,尽管它们在垂体切除的大鼠中表达不依赖于GH。此外,新生期MSG处理,特别是在雌性大鼠中,可能导致除GH之外的其他因子丧失,而这些因子是脉冲式GH刺激的CYP 2A2、3A2和2C11基因充分表达所必需的。
