首页> 美国卫生研究院文献>The Journal of Physiology >Robust L-type calcium current expression following heterozygous knockout of the Cav1.2 gene in adult mouse heart
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Robust L-type calcium current expression following heterozygous knockout of the Cav1.2 gene in adult mouse heart

机译:Cav1.2基因杂合敲除后在成年小鼠心脏中的强大L型钙电流表达

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摘要

Non-technical summaryAppropriate regulation of ion channel expression is critical for the maintenance of both electrical stability and normal contractile function in the heart. A classic way to study the robustness of biological systems is to examine the effects of changes in gene dosage. We have studied how the heart responds to changes in the L-type calcium channel gene dosage. Homozygous Cav1.2 knockout in the adult heart is lethal, without compensatory responses in expression of other calcium channel genes. Following heterozygous knockout, Cav1.2 mRNA levels are not buffered, Cav1.2 membrane protein levels are partly buffered and L-type calcium current expression is relatively well buffered. These data are consistent with a passive model of Cav1.2 biosynthesis that includes saturated steps, which act to buffer Cav1.2 protein and L-type calcium current expression. The results suggest that there is little or no homeostatic regulation of calcium current expression in either heterozygous or homozygous knockout mice.
机译:非技术摘要适当调节离子通道的表达对于维持心脏的电稳定性和正常收缩功能至关重要。研究生物系统健壮性的经典方法是检查基因剂量变化的影响。我们研究了心脏如何响应L型钙通道基因剂量的变化。在成年心脏中纯合的Cav1.2基因敲除是致命的,其他钙通道基因的表达没有补偿反应。杂合敲除后,Cav1.2 mRNA水平不被缓冲,Cav1.2膜蛋白水平被部分缓冲,L型钙电流表达相对被缓冲。这些数据与Cav1.2生物合成的被动模型一致,该模型包括饱和步骤,可起到缓冲Cav1.2蛋白和L型钙电流表达的作用。结果表明,在杂合或纯合敲除小鼠中,钙电流表达几乎没有或没有稳态调节。

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