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Middle-age alterations in the sexually dimorphic plasma growth hormone profiles: involvement of growth hormone-releasing factor and effects on cytochrome p450 expression.

机译:性双态血浆生长激素谱中的中年变化:生长激素释放因子的参与和对细胞色素p450表达的影响。

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摘要

Rat liver, as well as other species, contains numerous sex-dependent isoforms of cytochrome P450 (P450) that are regulated by the sexually dimorphic profiles of circulating growth hormone. During puberty, young adulthood, and senescence, changes in the hormonal profiles appear to be responsible for alterations in age-associated expression levels of selective P450 isoforms. In contrast, little is known about the growth hormone secretory profiles and their P450-dependent expression levels during middle age. In the present study, we observed subtle changes in the hormonal concentrations, and frequencies of peaks and interpulse periods in the sexually dimorphic growth hormone profiles of 1-year-old male and female rats correlated to suppression of male-specific isoforms CYP2C11 and CYP2C13 and female-predominant CYP2C7. To identify possible causes for the age-associated changes in the circulating growth hormone profiles, the responsiveness of the hypothalamic-pituitary axis to growth hormone secretagogues clonidine and growth hormone-releasing factor (GRF) were examined in middle-aged male and female rats. In spite of the same sexually dimorphic response in young adult and middle-aged rats to both secretogogues (males > females), the pituitary somatotrophs in the older animals exhibited a dramatic decrease in sensitivity to clonidine, characterized by subnormal growth hormone release levels and an inordinate delay in pituitary response to clonidine stimulation. Results from similar studies conducted on middle-aged arcuate nucleus-lesioned rats suggest that a decline in GRF secretion is a possible contributor to the age-associated alterations in plasma growth hormone profiles during middle age. These changes in GRF-induced, sexually dimorphic secretory growth hormone profiles and the accompanying decline in P450 expression levels may anticipate similar, but more profound, changes to occur during senescence.
机译:大鼠肝脏以及其他物种,都包含许多细胞色素P450(P450)的性别依赖性同工型,这些同工型受循环生长激素的性二态性状调控。在青春期,成年和衰老期间,激素谱的变化似乎是选择性P450异构体与年龄相关的表达水平改变的原因。相反,对中年时期生长激素分泌特征及其P450依赖性表达水平知之甚少。在本研究中,我们观察到1岁雄性和雌性大鼠的性二态性生长激素谱中激素浓度的微妙变化以及峰值和间断周期的频率与抑制雄性特异性同工型CYP2C11和CYP2C13和女性为主要的CYP2C7。为了确定循环生长激素谱中与年龄相关的变化的可能原因,在中年雄性和雌性大鼠中检查了下丘脑-垂体轴对生长激素促泌剂可乐定和生长激素释放因子(GRF)的反应。尽管年轻成年和中年大鼠对两种促分泌激素的性双态反应相同(雄性>雌性),但老年动物的垂体生长激素对可乐定的敏感性却显着降低,其特征在于生长激素释放水平不正常,并且对可乐定刺激垂体反应的过度延迟。对中年弓形核损伤大鼠进行的类似研究的结果表明,GRF分泌减少可能是中年血浆生长激素谱与年龄相关的变化的原因。 GRF诱导的,性二态性分泌生长激素谱的这些变化以及伴随的P450表达水平的下降可能预期在衰老过程中会发生相似但更深刻的变化。

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