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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Protective effects of exercise and phosphoinositide 3-kinase(p110 alpha) signaling in dilated and hypertrophic cardiomyopathy
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Protective effects of exercise and phosphoinositide 3-kinase(p110 alpha) signaling in dilated and hypertrophic cardiomyopathy

机译:运动和磷酸肌醇3-激酶(p110 alpha)信号传导对扩张型和肥厚型心肌病的保护作用

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摘要

Physical activity protects against cardiovascular disease, and physiological cardiac hypertrophy associated with regular exercise is usually beneficial, in marked contrast to pathological hypertrophy associated with disease. The p110 alpha isoform of phosphoinositide 3-kinase (PI3K) plays a critical role in the induction of exercise-induced hypertrophy. Whether it or other genes activated in the athlete's heart might have an impact on cardiac function and survival in a setting of heart failure is unknown. To examine whether progressive exercise training and PI3K(p110 alpha) activity affect survival and/or cardiac function in two models of heart disease, we subjected a transgenic mouse model of dilated cardiomyopathy (DCM) to swim training, genetically crossed cardiac-specific transgenic mice with increased or decreased PI3K(p110 alpha) activity to the DCM model, and subjected PI3K(p110 alpha) transgenics to acute pressure overload (ascending aortic constriction). Life span, cardiac function, and molecular markers of pathological hypertrophy were examined. Exercise training and increased cardiac PI3K(p110 alpha) activity prolonged survival in the DCM model by 15-20%. In contrast, reduced PI3K(p110 alpha) activity drastically shortened lifespan by approximate to 50%. Increased PI3K(p110 alpha) activity had a favorable effect on cardiac function and fibrosis in the pressure-overload model and attenuated pathological growth. PI3K(p110 alpha) signaling negatively regulated G protein-coupled receptor stimulated extracellular responsive kinase and Akt (via PI3K, p110 gamma) activation in isolated cardiomyocytes. These findings suggest that exercise and enhanced PI3K(p110 alpha) activity delay or prevent progression of heart disease, and that supraphysiologic activity can be beneficial. Identification of genes important for hypertrophy in the athlete's heart could offer new strategies for treating heart failure.
机译:进行体育锻炼可预防心血管疾病,与疾病相关的病理性肥大形成鲜明对比,经常运动引起的生理性心脏肥大通常是有益的。磷酸肌醇3-激酶(PI3K)的p110α亚型在诱导运动引起的肥大中起关键作用。它或运动员心脏中激活的其他基因是否可能对心功能和心力衰竭患者的生存产生影响尚不清楚。若要检查进行性运动训练和PI3K(p110 alpha)活性是否会影响两种心脏病模型的存活和/或心脏功能,我们对扩张型心肌病(DCM)的转基因小鼠模型进行了游泳训练,并进行了遗传杂交的心脏特异性转基因小鼠与DCM模型相比,PI3K(p110 alpha)活性升高或降低,并使PI3K(p110 alpha)转基因遭受急性压力超负荷(升主动脉缩窄)。检查寿命,心脏功能和病理性肥大的分子标记。运动训练和增加心脏PI3K(p110 alpha)活性可使DCM模型的生存期延长15-20%。相反,降低的PI3K(p110 alpha)活性将使寿命大大缩短大约50%。 PI3K(p110 alpha)活性的增加对压力超负荷模型中的心脏功能和纤维化具有良好的作用,并减弱了病理性生长。 PI3K(p110 alpha)信号指示负调控的G蛋白偶联受体刺激离体心肌细胞中的细胞外应答激酶和Akt(通过PI3K,p110γ)活化。这些发现表明,锻炼和增强PI3K(p110 alpha)活性可以延迟或预防心脏病的发展,超生理活性可能是有益的。鉴定对运动员心脏肥大重要的基因可能为治疗心力衰竭提供新的策略。

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