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使用秩图分析和随机血样探索小鼠的内分泌 GH 模式。

Exploring endocrine GH pattern in mice using rank plot analysis and random blood samples.

机构信息

INSERM U938, Hôpital Saint-Antoine, Bâtiment Kourilsky, 184 rue du Faubourg Saint-Antoine, F-75012 Paris, France.

出版信息

J Endocrinol. 2011 Feb;208(2):119-29. doi: 10.1677/JOE-10-0317. Epub 2010 Nov 2.

DOI:10.1677/JOE-10-0317
PMID:21045135
Abstract

GH plays important pleiotropic roles in development, growth, metabolism, and aging of vertebrate species. Mouse mutants with altered GH signaling have been increasingly instrumental in studying somatotropic pathophysiology. However, the pulsatile characteristics of GH secretion are difficult to study in mice because catheterization is cumbersome and long-term serial sampling is limited by small body size and blood volume. We therefore developed an approach routinely applicable to mice, which detects endogenous, physiological GH pattern from randomly obtained spot samples. We determined individual hormone concentration in large groups of mice, ranked the data by magnitude, and statistically analyzed the resulting profiles. This revealed that the nadir-to-peak distribution of plasma GH concentration in mice was similar to other mammals, and that nycthemeral and sex differences existed as well. We found handling stress to be a potent immediate downregulator of circulating GH. We showed that samples need to be taken within seconds to reflect true endogenous levels, unaffected by stress. GH receptor/Janus kinase 2/signal transducer and activator of transcription 5 activation measured in the liver correlated strongly with plasma GH levels, but peak concentrations did not further increase the pathway activation. We applied this rank plot analysis to the GH-deficient and long-lived brain-specific IGF-1 receptor knockout (bIGF1RKO(+/-)) mouse mutant and found a high proportion of low GH concentrations, indicative of extended trough periods and rare peaks. Taken together, we showed that rank plot analysis is a useful method that allows straightforward studies of circadian endogenous GH levels in mice.

摘要

生长激素在脊椎动物物种的发育、生长、代谢和衰老中发挥着重要的多效作用。改变生长激素信号的小鼠突变体在研究躯体生理学方面越来越重要。然而,由于置管繁琐,并且由于体型小和血量有限,长期进行系列采样受到限制,因此难以研究生长激素分泌的脉冲特征。因此,我们开发了一种常规适用于小鼠的方法,该方法可以从随机获得的点样中检测内源性生理生长激素模式。我们确定了大量小鼠个体的激素浓度,按大小对数据进行排序,并对所得图谱进行了统计分析。这表明,小鼠血浆生长激素浓度的低谷到峰值分布与其他哺乳动物相似,并且存在昼夜和性别差异。我们发现处理应激是循环生长激素的有效即时下调因子。我们表明,需要在几秒钟内采集样本,以反映不受应激影响的真实内源性水平。肝脏中测量的生长激素受体/Janus 激酶 2/信号转导和转录激活物 5 激活与血浆生长激素水平密切相关,但峰值浓度不会进一步增加该途径的激活。我们将这种等级图分析应用于生长激素缺乏和长寿的脑特异性 IGF-1 受体敲除(bIGF1RKO(+/-))小鼠突变体,并发现了大量低生长激素浓度,表明低谷期延长和峰值罕见。总之,我们表明等级图分析是一种有用的方法,可以直接研究小鼠的昼夜内源性生长激素水平。

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