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运动对钠/氢交换蛋白过表达小鼠心脏病理学的性别特异性影响。

Gender-specific effects of exercise on cardiac pathology in Na(+)/H(+) exchanger overexpressing mice.

机构信息

Department of Biochemistry, University Alberta, Edmonton, AB T6G 2H7, Canada.

出版信息

Mol Cell Biochem. 2012 Sep;368(1-2):103-10. doi: 10.1007/s11010-012-1348-1. Epub 2012 May 25.

Abstract

The Na(+)/H(+) exchanger isoform 1 (NHE1) has been implicated in various cardiac pathologies including ischemia/reperfusion damage to the myocardium and cardiac hypertrophy. It is known that NHE1 levels increase in cardiac disease and we have recently demonstrated that expression of an activated NHE1 protein promotes cardiac hypertrophy in the mouse myocardium. We examined the gender-specific effects of exercise in combination with elevated cardiac expression of NHE1 on the myocardium in mice. Control mice and transgenic mice expressing elevated levels of wild type NHE1 and activated NHE1 were examined. There were gender-specific differences in the effects of NHE1 with exercise. Exercised wild type male mice showed a tendency toward increased heart weight. This was not apparent in female mice expressing elevated NHE1 levels. In some transgenic female mice, there was a significant decrease in the size of the exercised hearts, which was different from what occurred with male mice. Body weight was maintained in exercised control and transgenic male mice; however, it decreased in female mice with exercise more so in transgenic female mice expressing elevated levels of NHE1. Female mice expressing activated NHE1 had elevated HW/BW ratios compared to males, and this was exaggerated by exercise. These results suggest that gender-specific activation of NHE1 may be critical and that NHE1 plays a more critical role in promoting some types of hypertrophy in females in comparison with males.

摘要

钠/氢交换体亚型 1(NHE1)已被牵涉到多种心脏病理变化,包括心肌的缺血/再灌注损伤和心脏肥大。已知 NHE1 水平在心脏疾病中增加,我们最近证明,激活的 NHE1 蛋白的表达促进了小鼠心肌中的心脏肥大。我们研究了运动与心脏中 NHE1 水平升高对小鼠心肌的性别特异性影响。检查了表达高水平野生型 NHE1 和激活型 NHE1 的转基因小鼠的对照小鼠和转基因小鼠。NHE1 的作用存在性别特异性差异,运动对其有影响。运动的野生型雄性小鼠的心脏重量有增加的趋势。而在表达升高的 NHE1 水平的雌性小鼠中,这并不明显。在一些转基因雌性小鼠中,运动后的心脏明显缩小,这与雄性小鼠的情况不同。运动后的对照和转基因雄性小鼠的体重保持不变;然而,运动后雌性小鼠的体重下降,在表达高水平 NHE1 的转基因雌性小鼠中更为明显。表达激活型 NHE1 的雌性小鼠的 HW/BW 比值高于雄性,而运动则使这种比值进一步升高。这些结果表明,NHE1 的性别特异性激活可能是关键的,并且 NHE1 在促进女性某些类型的肥大方面比男性更为重要。

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