首页> 外文期刊>Neuroendocrinology: International Journal for Basic and Clinical Studies on Neuroendocrine Relationships >Hypophysiotropic somatostatin expression during postnatal development in growth hormone-deficient Ames dwarf mice: mRNA in situ hybridization.
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Hypophysiotropic somatostatin expression during postnatal development in growth hormone-deficient Ames dwarf mice: mRNA in situ hybridization.

机译:生长激素缺乏型Ames矮小鼠出生后发育过程中的促生长素生长抑素表达:mRNA原位杂交。

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摘要

Lifelong deficiency of growth hormone (GH) in spontaneous or transgenic dwarf mice has been shown to be accompanied by reduced hypophysiotropic somatostatin (somatotropin release-inhibiting hormone, SRIH) expression in hypothalamic anterior periventricular nucleus (PeN). However, the postnatal developmental pattern of SRIH expression in the absence of GH is unknown. Therefore, SRIH mRNA levels in GH-deficient Ames dwarf (df/df) mice and normal (DF/?) littermates were determined both in adults, to compare with other GH-deficient models, and at selected days of postnatal development, to determine the effects of GH deficiency on SRIH neuron development. DF/? and df/df mice of both sexes at postnatal ages 1, 3, 7, 14, 21 and 60 days (adult) were examined. In situ hybridization and image analysis were used to quantify the relative abundance of total SRIH mRNA in the PeN, and SRIH mRNA per cell was determined in PeN and medial basal hypothalamus (MBH). In adult df/df mice, total PeN SRIH mRNA was 45% (p < 0.05) of that in DF/? littermates, which is consistent with studies of other GH-deficient dwarf mice. In developing animals, SRIH expression in the PeN of DF/? mice began at 3 days of age and increased at subsequent ages to reach adult levels. In df/df mice, PeN SRIH mRNA levels at 60 days were significantly greater than at 1-21 days of age (p < 0.05). However, levels were not different over 1-21 days of age, and were consistently lower in df/df than DF/? mice. The difference in total PeN SRIH mRNA between df/df and DF/? mice was statistically significant at 7 days, and at each subsequent age. There were no differences between DF/? and df/df mice in the number of grains per cell in either PeN or MBH at any age. Thus, the reduced total hypophysiotropic SRIH mRNA in GH-deficient Ames dwarf mice appears developmentally shortly after initial detectability of SRIH in the PeN. Because SRIH mRNA per cell was the same for DF/? and df/df mice, the decreased total mRNA in dwarfs suggested reduced SRIH cell numbers in PeN, which was corroborated by immunocytochemical findings. The reduction of SRIH in df/df mice at 7 days of age suggests that GH production during embryonic or very early postnatal development is important to activation of PeN SRIH transcription.
机译:自发性或转基因矮化小鼠终生缺乏生长激素(GH)伴随着下丘脑前脑室前核(PeN)的促生长激素生长抑素(生长激素释放抑制激素,SRIH)表达降低。然而,在不存在GH的情况下,SRIH表达的产后发育模式是未知的。因此,要确定成年GH缺陷的Ames矮人(df / df)小鼠和正常(DF /?)同窝仔小鼠的SRIH mRNA水平,以便与其他GH缺陷模型进行比较,并在出生后的选定几天确定生长激素缺乏症对SRIH神经元发育的影响。 DF /?检查了出生后1、3、7、14、21和60天(成人)的雌雄同体的df / df和df / df小鼠。原位杂交和图像分析用于定量PeN中总SRIH mRNA的相对丰度,并在PeN和内侧下丘脑(MBH)中确定每个细胞的SRIH mRNA。在成年df / df小鼠中,PeN SRIH mRNA的总含量为DF /?的45%(p <0.05)。同窝仔,这与其他GH缺乏矮人小鼠的研究一致。在发育中的动物中,SRIH在DF /β的PeN中表达。小鼠在3天大时开始,并在随后的年龄增加到成年水平。在df / df小鼠中,第60天的PeN SRIH mRNA水平显着高于1-21天的年龄(p <0.05)。但是,在1至21天的年龄中水平没有差异,并且df / df始终低于DF /?。老鼠。 df / df和DF /?之间的总PeN SRIH mRNA差异小鼠在第7天及以后的每个年龄段均有统计学意义。 DF /之间没有区别。和df / df小鼠在任何年龄的PeN或MBH中每个细胞的粒数。因此,GH缺陷的Ames矮小鼠的总促生理SRIH mRNA降低,在PeN中最初检测到SRIH之后不久就出现了发育。因为每个细胞的SRIH mRNA对于DF /α是相同的。对于df / df和df / df小鼠,矮人中的总mRNA降低表明PeN中SRIH细胞数量减少,这通过免疫细胞化学结果得到证实。 df / df小鼠在7天龄时SRIH的减少表明,胚胎期或出生后早期发育过程中GH的产生对于激活PeN SRIH转录很重要。

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