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丹曲林对哺乳动物骨骼肌纤维兴奋-收缩偶联步骤的影响。

Effects of dantrolene on steps of excitation-contraction coupling in mammalian skeletal muscle fibers.

作者信息

Szentesi P, Collet C, Sárközi S, Szegedi C, Jona I, Jacquemond V, Kovács L, Csernoch L

机构信息

Department of Physiology, Medical and Health Science Center, University of Debrecen, Debrecen, Hungary, H-4012.

出版信息

J Gen Physiol. 2001 Oct;118(4):355-75. doi: 10.1085/jgp.118.4.355.

Abstract

The effects of the muscle relaxant dantrolene on steps of excitation-contraction coupling were studied on fast twitch muscles of rodents. To identify the site of action of the drug, single fibers for voltage-clamp measurements, heavy SR vesicles for calcium efflux studies and solubilized SR calcium release channels/RYRs for lipid bilayer studies were isolated. Using the double Vaseline-gap or the silicone-clamp technique, dantrolene was found to suppress the depolarization-induced elevation in intracellular calcium concentration ([Ca2+]i) by inhibiting the release of calcium from the SR. The suppression of [Ca2+]i was dose-dependent, with no effect at or below 1 microM and a 53 +/- 8% (mean +/- SEM, n = 9, cut fibers) attenuation at 0 mV with 25 microM of extracellularly applied dantrolene. The drug was not found to be more effective if injected than if applied extracellularly. Calculating the SR calcium release revealed an equal suppression of the steady (53 +/- 8%) and of the early peak component (46 +/- 6%). The drug did not interfere with the activation of the voltage sensor in as much as the voltage dependence of both intramembrane charge movements and the L-type calcium currents (I(Ca)) were left, essentially, unaltered. However, the inactivation of I(Ca) was slowed fourfold, and the conductance was reduced from 200 +/- 16 to 143 +/- 8 SF(-1) (n = 10). Dantrolene was found to inhibit thymol-stimulated calcium efflux from heavy SR vesicles by 44 +/- 10% (n = 3) at 12 microM. On the other hand, dantrolene failed to affect the isolated RYR incorporated into lipid bilayers. The channel displayed a constant open probability for as long as 30-50 min after the application of the drug. These data locate the binding site for dantrolene to be on the SR membrane, but be distinct from the purified RYR itself.

摘要

在啮齿动物的快肌上研究了肌肉松弛剂丹曲林对兴奋 - 收缩偶联步骤的影响。为确定药物的作用位点,分离出用于电压钳测量的单纤维、用于钙外流研究的重肌浆网(SR)囊泡以及用于脂质双层研究的溶解的SR钙释放通道/雷诺丁受体(RYR)。使用双凡士林间隙或硅胶钳技术,发现丹曲林通过抑制SR中钙的释放来抑制去极化诱导的细胞内钙浓度([Ca2+]i)升高。[Ca2+]i的抑制呈剂量依赖性,在1 microM及以下浓度时无作用,在0 mV时,细胞外施加25 microM丹曲林时抑制率为53±8%(平均值±标准误,n = 9,切断的纤维)。未发现药物注射比细胞外应用更有效。计算SR钙释放显示,稳态成分(53±8%)和早期峰值成分(46±6%)受到同等程度的抑制。药物并不干扰电压传感器的激活,因为膜内电荷移动和L型钙电流(I(Ca))的电压依赖性基本保持不变。然而,I(Ca)的失活减慢了四倍,电导率从200±16降至143±8 SF(-1)(n = 10)。发现丹曲林在12 microM时可抑制百里酚刺激的重SR囊泡中的钙外流44±10%(n = 3)。另一方面,丹曲林未能影响整合到脂质双层中的分离的RYR。在应用药物后长达30 - 50分钟内,通道显示出恒定的开放概率。这些数据表明丹曲林的结合位点位于SR膜上,但与纯化的RYR本身不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e796/2233700/9f24f1e41e4f/JGP8403.f1.jpg

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