首页> 美国卫生研究院文献>Biochemical Journal >Functional development of sex accessory organs of the male rat. Use of oestradiol benzoate to identify the neonatal period as critical for development of normal protein-synthetic and secretory capabilities.
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Functional development of sex accessory organs of the male rat. Use of oestradiol benzoate to identify the neonatal period as critical for development of normal protein-synthetic and secretory capabilities.

机译:雄性大鼠性附属器官的功能发育。使用雌二醇苯甲酸酯来确定新生儿时期对于正常蛋白质合成和分泌能力的发展至关重要。

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摘要

Functional development of the sex accessory tissues was studied in the male rat. Three potentially crucial developmental periods (neonatal, prepubertal and pubertal) were examined, and then the functional integrity of the accessory tissues was investigated in the adult, when the animals would have been expected to display normal function. Four accessory tissues (the seminal vesicles, ventral prostate and caput and cauda epididymides) were used because of their different embryological origins and responses to androgens in the adult. Synthesis and secretion of previously characterized tissue-specific androgen-dependent proteins were taken as indicators of normal function. Development was perturbed by using oestradiol benzoate, since this was known to affect gross development of the seminal vesicles and ventral prostate when given to neonatal rats. Treatment during the first 5 days after birth severely restricted development of the seminal vesicles and ventral prostate. Protein secreted by the former was only 1% of the normal amount, and in many cases several major secretory proteins were essentially missing. Prostatic protein secretion was less than 20% of normal, but all the major proteins were detectable. In both tissues overall protein synthesis per cell was quantitatively normal, but the proportion devoted to specific major secretory proteins was markedly depressed, i.e. the response is differential. In contrast, treatment during the prepubertal period was without noticeable effects. Development of the seminal vesicles and prostate was somewhat inhibited by treatment at puberty, but these changes were minor compared with those after neonatal exposure to oestradiol benzoate. No effects on epididymal protein synthesis or secretory proteins were observed, and epididymal weight and DNA content were only moderately decreased regardless of when oestradiol benzoate was administered during sexual maturation. Hence the neonatal period is not so critical for epididymal development. The substantial changes elicited by oestrogen treatment during neonatal life in seminal-vesicle and prostatic protein synthesis and secretion were compared with those evoked in sexually mature males by either oestrogen treatment or castration. Both these latter treatments resulted in a general decrease in seminal-vesicle protein synthesis and secretion, but the marked differential effects on major proteins after neonatal exposure were absent. Castration did, however, evoke a differential prostatic response, but this was not seen after oestrogen treatment of adults.
机译:在雄性大鼠中研究了性附属组织的功能发育。检查了三个潜在的关键发育时期(新生儿,青春期和青春期),然后研究了成年动物中附属组织的功能完整性,那时这些动物有望表现出正常的功能。使用了四个辅助组织(精囊,腹侧前列腺和角膜和附睾),因为它们的胚胎起源不同,并且对成年雄激素的反应也不同。先前表征的组织特异性雄激素依赖性蛋白的合成和分泌被视为正常功能的指标。使用雌二醇苯甲酸酯会干扰发育,因为已知这会影响新生大鼠的精囊和腹侧前列腺的总体发育。出生后头5天的治疗严重限制了精囊和腹侧前列腺的发育。前者分泌的蛋白质仅为正常量的1%,而且在许多情况下,基本上缺少几种主要的分泌蛋白质。前列腺蛋白质的分泌少于正常蛋白质的20%,但所有主要蛋白质均可检出。在两个组织中,每个细胞的总体蛋白质合成在数量上是正常的,但是专门用于特定主要分泌蛋白的比例明显降低,即反应是不同的。相反,青春期前的治疗效果不明显。青春期治疗对精囊和前列腺的发育有一定的抑制作用,但与新生儿暴露于雌二醇苯甲酸酯后相比,这些变化很小。没有观察到对附睾蛋白质合成或分泌蛋白质的影响,并且不论性成熟期间何时施用雌二醇苯甲酸酯,附睾重量和DNA含量仅适度降低。因此,新生儿期对于附睾的发展并不是那么关键。将雌激素治疗在新生儿生命中精囊和前列腺蛋白质合成和分泌中引起的实质性变化与通过雌激素治疗或去势在性成熟男性中诱发的变化进行了比较。后两种治疗均导致精囊蛋白合成和分泌普遍下降,但新生儿暴露后对主要蛋白没有明显的差别作用。然而,去势确实引起了不同的前列腺反应,但这在成人的雌激素治疗后未见到。

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