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年龄和胰岛素样生长因子-I给药对大鼠主动脉弹性蛋白基因表达的影响。

Effect of age and IGF-I administration on elastin gene expression in rat aorta.

作者信息

Foster J A, Rich C B, Miller M, Benedict M R, Richman R A, Florini J R

机构信息

Department of Biology, Syracuse University, New York.

出版信息

J Gerontol. 1990 Jul;45(4):B113-8. doi: 10.1093/geronj/45.4.b113.

DOI:10.1093/geronj/45.4.b113
PMID:1694873
Abstract

An age-related decrease in elasticity of arteries has been found in clinical and experimental studies done during the past two decades. We have investigated molecular and endocrine aspects of that decrease by examining the effects of age and insulin-like growth factor-I (IGF-I) on rat aorta elastogenesis. For comparison, pulmonary elastogenesis was examined in the same experimental animals. Different aged groups of male Fischer 344 rats (barrier protected) were implanted with minipumps for a two-week infusion of either 0.1 N acetic acid (vehicle solution) or IGF-I (1.2 mg/kg/day). The DNA content (micrograms DNA/g tissue) decreased with age in aorta but remained fairly constant in lung. Administration of IGF-I increased the aortic DNA content in all but the oldest rats. Conversely, the DNA content of pulmonary tissue was significantly increased in only the youngest animals. The steady-state levels of tropoelastin mRNA decreased dramatically in both aorta and lung with increased age. The decrease was greater in lung than aorta. Administration of IGF-I elevated aortic tropoelastin mRNA steady-state levels, whereas lung tropoelastin mRNA levels were unaffected by IGF-I administration. Aortic tissue synthesized decreased amounts of insoluble elastin with increased age. These results establish a direct relationship between aortic tropoelastin mRNA levels and the synthesis of insoluble elastin in aging. Administration of IGF-I increased aortic elastin synthesis throughout the life span of the rat, although the proportionate increase diminished with age.

摘要

在过去二十年进行的临床和实验研究中,已发现动脉弹性随年龄增长而降低。我们通过研究年龄和胰岛素样生长因子-I(IGF-I)对大鼠主动脉弹性生成的影响,来探究这种降低的分子和内分泌方面。为作比较,在相同的实验动物中检查了肺弹性生成。将不同年龄组的雄性Fischer 344大鼠(屏障保护)植入微型泵,以两周时间输注0.1N乙酸(赋形剂溶液)或IGF-I(1.2mg/kg/天)。主动脉中的DNA含量(微克DNA/克组织)随年龄增长而降低,但肺中的DNA含量保持相当恒定。给予IGF-I后,除最老的大鼠外,所有大鼠的主动脉DNA含量均增加。相反,仅最年轻的动物肺组织的DNA含量显著增加。随着年龄增长,主动脉和肺中原弹性蛋白mRNA的稳态水平均显著降低。肺中的降低幅度大于主动脉。给予IGF-I可提高主动脉原弹性蛋白mRNA的稳态水平,而肺原弹性蛋白mRNA水平不受IGF-I给药的影响。随着年龄增长,主动脉组织合成的不溶性弹性蛋白量减少。这些结果确立了衰老过程中主动脉原弹性蛋白mRNA水平与不溶性弹性蛋白合成之间的直接关系。在大鼠的整个生命周期中,给予IGF-I均可增加主动脉弹性蛋白的合成,尽管随着年龄增长,成比例的增加幅度会减小。

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