Department of Biological Sciences, California State Polytechnic University, Pomona, CA 91768, USA.
Proc Natl Acad Sci U S A. 2013 May 28;110(22):9160-5. doi: 10.1073/pnas.1220068110. Epub 2013 May 13.
Huntington disease is a progressive and fatal genetic disorder with debilitating motor and cognitive defects. Chorea, rigidity, dystonia, and muscle weakness are characteristic motor defects of the disease that are commonly attributed to central neurodegeneration. However, no previous study has examined the membrane properties that control contraction in Huntington disease muscle. We show primary defects in ex vivo adult skeletal muscle from the R6/2 transgenic mouse model of Huntington disease. Action potentials in diseased fibers are more easily triggered and prolonged than in fibers from WT littermates. Furthermore, some action potentials in the diseased fibers self-trigger. These defects occur because of decreases in the resting chloride and potassium conductances. Consistent with this, the expression of the muscle chloride channel, ClC-1, in Huntington disease muscle was compromised by improper splicing and a corresponding reduction in total Clcn1 (gene for ClC-1) mRNA. Additionally, the total Kcnj2 (gene for the Kir2.1 potassium channel) mRNA was reduced in disease muscle. The resulting muscle hyperexcitability causes involuntary and prolonged contractions that may contribute to the chorea, rigidity, and dystonia that characterize Huntington disease.
亨廷顿舞蹈病是一种进行性和致命的遗传性疾病,会导致运动和认知功能受损。舞蹈症、僵硬、肌张力障碍和肌肉无力是该疾病的典型运动缺陷,通常归因于中枢神经退行性变。然而,以前没有研究检查过控制亨廷顿病肌肉收缩的膜特性。我们显示了来自亨廷顿病 R6/2 转基因小鼠模型的体外成年骨骼肌的主要缺陷。与 WT 同窝仔的纤维相比,患病纤维中的动作电位更容易被触发且持续时间更长。此外,患病纤维中的一些动作电位会自动触发。这些缺陷是由于静息氯离子和钾离子电导率降低所致。与此一致的是,肌肉氯离子通道 ClC-1 的表达因剪接不当和总 Clcn1(ClC-1 基因)mRNA 的相应减少而受损。此外,疾病肌肉中的总 Kcnj2(Kir2.1 钾通道基因)mRNA 减少。由此产生的肌肉过度兴奋导致不自主和长时间的收缩,这可能导致亨廷顿舞蹈病的舞蹈症、僵硬和肌张力障碍等特征。