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对注射了来自大鼠心脏的mRNA的非洲爪蟾卵母细胞中表达的电压依赖性钙通道的特性分析。

Characterization of voltage-dependent calcium channels expressed in Xenopus oocytes injected with mRNA from rat heart.

作者信息

Lory P, Rassendren F A, Richard S, Tiaho F, Nargeot J

机构信息

Centre de Recherches de Biochimie Macromoléculaire, UPR 8402 CNRS, U 249 INSERM, Montpellier, France.

出版信息

J Physiol. 1990 Oct;429:95-112. doi: 10.1113/jphysiol.1990.sp018246.

Abstract
  1. The properties of voltage dependent cardiac Ca channels expressed in Xenopus laevis oocytes after injection of mRNA from rat heart were investigated using the double-microelectrode voltage-clamp technique. 2. Endogenous Ba current (IBa,E) and expressed cardiac Ba current (IBa,C) were studied at various external concentrations of barium (Ba2+). These two entities could be distinguished by their amplitude and their pharmacology. IBa,C was more sensitive to the inorganic Ca channel blocker manganese (Mn2+). The contaminant IBa,E presented properties of voltage dependence identical to IBa,C, but was negligible in the presence of a low external Ba2+ concentration (2 mM). 3. In 2 mM-Ba2+, IBa,C activated at -35 mV, peaked at -14 mV, and reversed at +26 mV. Steady-state inactivation properties, in consideration of the half-inactivation potential of -35 mV, were also typical of L-type Ba currents. However, the decay of IBa,C was very slow (time constant of inactivation near 600 ms). No evidence for the expression of cardiac transient Ca channels (T-type) was found. 4. IBa,C was enhanced after exposure to the 1,4-dihydropyridine (DHP) agonist Bay K 8644. The enhancement of IBa,C was voltage dependent (maximum at -30 +/- 5 mV) and associated with a slowing in current decay. Current-voltage and concentration-response curves obtained for various Ba2+ concentrations revealed an antagonism between external Ba2+ and the 1,4-DHP agonist Bay K 8644. Similar results were found using the (-)Bay K 8644 pure agonist isomer. 5. We conclude that oocytes injected with mRNA from rat heart expressed only the high threshold, long-lasting or L-type Ca channels. The availability of expressed L-type Ca channels for quantitative pharmacological studies using low Ba2+ concentration has been demonstrated.
摘要
  1. 运用双微电极电压钳技术,研究了注射大鼠心脏mRNA后非洲爪蟾卵母细胞中表达的电压依赖性心脏钙通道的特性。2. 在不同的细胞外钡(Ba2+)浓度下,研究了内源性钡电流(IBa,E)和表达的心脏钡电流(IBa,C)。这两种电流可通过其幅度和药理学特性加以区分。IBa,C对无机钙通道阻滞剂锰(Mn2+)更为敏感。污染性的IBa,E呈现出与IBa,C相同的电压依赖性特性,但在低细胞外Ba2+浓度(2 mM)存在时可忽略不计。3. 在2 mM - Ba2+中,IBa,C在 - 35 mV时激活,在 - 14 mV时达到峰值,并在 + 26 mV时反转。考虑到半失活电位为 - 35 mV,其稳态失活特性也具有L型钡电流的典型特征。然而,IBa,C的衰减非常缓慢(失活时间常数接近600 ms)。未发现心脏瞬时钙通道(T型)表达的证据。4. 暴露于1,4 - 二氢吡啶(DHP)激动剂Bay K 8644后,IBa,C增强。IBa,C的增强具有电压依赖性(在 - 30 +/- 5 mV时最大),并伴有电流衰减减慢。针对不同Ba2+浓度获得的电流 - 电压和浓度 - 反应曲线显示,细胞外Ba2+与1,4 - DHP激动剂Bay K 8644之间存在拮抗作用。使用( - )Bay K 8644纯激动剂异构体也得到了类似结果。5. 我们得出结论,注射大鼠心脏mRNA的卵母细胞仅表达高阈值、持久的或L型钙通道。已证明使用低Ba2+浓度进行定量药理学研究时,表达的L型钙通道是可用的。

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