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新生儿和成年期性类固醇环境对下丘脑生长激素释放激素和生长抑素神经元的组织与激活的不同影响。

Differential effects of the neonatal and adult sex steroid environments on the organization and activation of hypothalamic growth hormone-releasing hormone and somatostatin neurons.

作者信息

Chowen J A, Argente J, González-Parra S, García-Segura L M

机构信息

Instituto Cajal, Consejo Superior de Investigaciones Científicas, Madrid, Spain.

出版信息

Endocrinology. 1993 Dec;133(6):2792-802. doi: 10.1210/endo.133.6.7902269.

Abstract

The secretory pattern of GH is markedly sexually dimorphic in the adult rat, a phenomenon that becomes manifest around the time of pubertal development. This event is due partially to the pubertal rise in gonadal steroids. However, the fetal and neonatal sex steroid environments also play an important role in generating this sexual dimorphism. Hypothalamic mRNA levels of GH-releasing hormone (GHRH) and somatostatin (SS), two neuropeptides implicated in the control of GH release, are sexually dimorphic in both neonatal and adult animals and, at least in the adult animal, are responsive to modulation by sex steroids. In this study, we examined the effects of neonatal testosterone on the number of GHRH and SS neurons in the adult hypothalamus as well as its effects on the responsivity of these neurons to later increases in sex steroids. To address these questions, male rats were either castrated or sham castrated on the day of birth (P0); these animals, along with intact females, received an injection of either testosterone or vehicle. At 60 days of age, half of each group received a Silastic capsule containing testosterone, and half received a sham implant. Growth rates were monitored throughout the study. At 75 days of age, animals were killed, and in situ hybridization to detect GHRH and SS mRNA containing neurons was performed. The number of GHRH neurons in the arcuate nucleus and ventromedial hypothalamus and the number of SS neurons in the periventricular nucleus and paraventricular nucleus were counted. Using a computerized image analysis system, GHRH and SS mRNA signal levels in individual neurons were also measured. Both neonatal and adult steroid treatments significantly increased growth rates. Those animals exposed to neonatal testosterone had significantly more detectable GHRH neurons than those that received only vehicle [P < 0.0001, by analysis of variance (ANOVA)]. Neonatal testosterone treatment had no effect on GHRH mRNA levels. Adult testosterone treatment, while having no effect on GHRH neuron numbers, stimulated GHRH mRNA levels in both males and females (P < 0.0001, ANOVA), but the magnitude of the increase depended upon whether the animal had been exposed to testosterone during the neonatal period. In contrast, the number of SS neurons was not affected by either steroid treatment. However, both treatments modulated SS mRNA levels (P < 0.0001, by ANOVA), with neonatal testosterone treatment alone resulting in significantly higher levels of SS mRNA in the adult animal. Adult testosterone treatment also significantly increased SS mRNA levels, and this was independent of previous exposure to sex steroids.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在成年大鼠中,生长激素(GH)的分泌模式具有明显的性别差异,这种现象在青春期发育前后变得明显。这一现象部分归因于青春期性腺类固醇的增加。然而,胎儿期和新生儿期的性类固醇环境在产生这种性别差异中也起着重要作用。生长激素释放激素(GHRH)和生长抑素(SS)是两种与GH释放控制有关的神经肽,它们在下丘脑的mRNA水平在新生动物和成年动物中都存在性别差异,并且至少在成年动物中,对性类固醇的调节有反应。在本研究中,我们研究了新生儿期睾酮对成年下丘脑GHRH和SS神经元数量的影响,以及其对这些神经元对后期性类固醇增加的反应性的影响。为了解决这些问题,雄性大鼠在出生当天(P0)进行阉割或假阉割;这些动物与未处理的雌性动物一起,接受睾酮或溶剂注射。在60日龄时,每组动物的一半接受含有睾酮的硅胶胶囊植入,另一半接受假植入。在整个研究过程中监测生长速率。在75日龄时,处死动物,并进行原位杂交以检测含有GHRH和SS mRNA的神经元。计数弓状核和腹内侧下丘脑的GHRH神经元数量以及室周核和室旁核的SS神经元数量。使用计算机图像分析系统,还测量了单个神经元中GHRH和SS mRNA的信号水平。新生儿期和成年期的类固醇处理均显著提高了生长速率。那些在新生儿期暴露于睾酮的动物比仅接受溶剂的动物有更多可检测到的GHRH神经元[方差分析(ANOVA),P < 0.0001]。新生儿期睾酮处理对GHRH mRNA水平没有影响。成年期睾酮处理虽然对GHRH神经元数量没有影响,但刺激了雄性和雌性动物的GHRH mRNA水平(ANOVA,P < 0.0001),但增加的幅度取决于动物在新生儿期是否暴露于睾酮。相比之下,两种类固醇处理均未影响SS神经元的数量。然而,两种处理均调节了SS mRNA水平(ANOVA,P < 0.0001),仅新生儿期睾酮处理就导致成年动物中SS mRNA水平显著升高。成年期睾酮处理也显著增加了SS mRNA水平,这与之前是否暴露于性类固醇无关。(摘要截断于400字)

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