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循环中胰岛素样生长因子-II水平升高的转基因小鼠的骨骼生长

Skeletal growth of transgenic mice with elevated levels of circulating insulin-like growth factor-II.

作者信息

Wolf E, Rapp K, Blum W F, Kolb H, Brem G

机构信息

Institut für Tierzucht und Genetik, Veterinärmedizinische Universität, Wien, Austria.

出版信息

Growth Regul. 1995 Dec;5(4):177-83.

PMID:8745142
Abstract

Insulin-like growth factor-II (IGF-II) is a major factor produced by skeletal tissues. To evaluate endocrine effects of IGF-II on bone growth, we measured skeletal dimensions of 12-week-old transgenic mice harbouring fusion genes where a human IGF-II cDNA is transcriptionally controlled by rat phospheonolpyruvate carboxykinase (PEPCK) promoter sequences. Transgene expression in liver, kidney and intestine resulted in circulating IGF-II levels in transgenic mice which were 2-3-fold higher than in controls. Serum IGF-I concentrations of transgenic mice were lower than in controls. Body weight was not influenced by the expression of the IGF-II transgene. Only 1 out of 5 measurements taken from the radius was significantly affected by the presence of the transgene, while in 60 measurements taken from eight other bones there was no difference between transgenic mice and controls. Furthermore, serum levels of calcium and phosphate as well as alkaline phosphatase activity were not significantly altered in PEPCK-IGF-II transgenic mice. Our findings demonstrate that moderately increased levels of circulating IGF-II do not cause major changes in skeletal growth and turnover in mice. This may be due to a lack of activity of circulating IGF-II on bone growth or to physiological consequences of elevated IGF-II, like a reduction of circulating IGF-I or an increase in IGF binding proteins.

摘要

胰岛素样生长因子-II(IGF-II)是骨骼组织产生的主要因子。为评估IGF-II对骨骼生长的内分泌作用,我们测量了携带融合基因的12周龄转基因小鼠的骨骼尺寸,该融合基因中人类IGF-II cDNA受大鼠磷酸烯醇丙酮酸羧激酶(PEPCK)启动子序列转录控制。肝脏、肾脏和肠道中的转基因表达导致转基因小鼠循环IGF-II水平比对照组高2至3倍。转基因小鼠的血清IGF-I浓度低于对照组。体重不受IGF-II转基因表达的影响。从桡骨进行的5次测量中只有1次受转基因存在的显著影响,而从其他八块骨头进行的60次测量中,转基因小鼠与对照组之间没有差异。此外,PEPCK-IGF-II转基因小鼠的血清钙、磷水平以及碱性磷酸酶活性没有显著改变。我们的研究结果表明,循环IGF-II水平适度升高不会引起小鼠骨骼生长和代谢的重大变化。这可能是由于循环IGF-II对骨骼生长缺乏活性,或者是IGF-II升高的生理后果,如循环IGF-I减少或IGF结合蛋白增加。

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