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发育不全的骨骼肌中的一种新型钙电流。

A novel calcium current in dysgenic skeletal muscle.

作者信息

Adams B A, Beam K G

机构信息

Department of Physiology, Colorado State University, Fort Collins 80523.

出版信息

J Gen Physiol. 1989 Sep;94(3):429-44. doi: 10.1085/jgp.94.3.429.

Abstract

The whole-cell patch-clamp technique was used to study voltage-dependent calcium currents in primary cultures of myotubes and in freshly dissociated skeletal muscle from normal and dysgenic mice. In addition to the transient, dihydropyridine (DHP)-insensitive calcium current previously described, a maintained DHP-sensitive calcium current was found in dysgenic skeletal muscle. This current, here termed ICa-dys, is largest in acutely dissociated fetal or neonatal dysgenic muscle and also in dysgenic myotubes grown on a substrate of killed fibroblasts. In dysgenic myotubes grown on untreated plastic culture dishes, ICa-dys is usually so small that it cannot be detected. In addition, ICa-dys is apparently absent from normal skeletal muscle. From a holding potential of -80 mV. ICa-dys becomes apparent for test pulses to approximately -20 mV and peaks at approximately +20 mV. The current activates rapidly (rise time approximately 5 ms at 20 degrees C) and with 10 mM Ca as charge carrier inactivates little or not at all during a 200-ms test pulse. Thus, ICa-dys activates much faster than the slowly activating calcium current of normal skeletal muscle and does not display Ca-dependent inactivation like the cardiac L-type calcium current. Substituting Ba for Ca as the charge carrier doubles the size of ICa-dys without altering its kinetics. ICa-dys is approximately 75% blocked by 100 nM (+)-PN 200-110 and is increased about threefold by 500 nM racemic Bay K 8644. The very high sensitivity of ICa-dys to these DHP compounds distinguishes it from neuronal L-type calcium current and from the calcium currents of normal skeletal muscle. ICa-dys may represent a calcium channel that is normally not expressed in skeletal muscle, or a mutated form of the skeletal muscle slow calcium channel.

摘要

采用全细胞膜片钳技术研究正常小鼠和发育不全小鼠原代培养肌管以及新鲜分离的骨骼肌中的电压依赖性钙电流。除了先前描述的瞬时、对二氢吡啶(DHP)不敏感的钙电流外,在发育不全的骨骼肌中还发现了一种持续存在的对DHP敏感的钙电流。这种电流,在此称为ICa-dys,在急性分离的胎儿或新生发育不全的肌肉以及在由灭活的成纤维细胞构成的基质上生长的发育不全肌管中最大。在未处理的塑料培养皿上生长的发育不全肌管中,ICa-dys通常非常小以至于无法检测到。此外,正常骨骼肌中显然不存在ICa-dys。从-80 mV的钳制电位开始,对于约-20 mV的测试脉冲,ICa-dys变得明显,并在约+20 mV时达到峰值。该电流快速激活(在20℃时上升时间约为5 ms),以10 mM Ca作为电荷载体时,在200 ms的测试脉冲期间几乎不发生或完全不发生失活。因此,ICa-dys的激活比正常骨骼肌缓慢激活的钙电流快得多,并且不像心脏L型钙电流那样表现出钙依赖性失活。用Ba替代Ca作为电荷载体可使ICa-dys的大小增加一倍,而不改变其动力学。ICa-dys约75%被100 nM(+)-PN 200-110阻断,并且被500 nM外消旋Bay K 8644增加约三倍。ICa-dys对这些DHP化合物的极高敏感性使其有别于神经元L型钙电流和正常骨骼肌的钙电流。ICa-dys可能代表一种通常不在骨骼肌中表达的钙通道,或者是骨骼肌慢钙通道的一种突变形式。

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