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Three components of the calcium current in cultured glomerulosa cells from rat adrenal gland.

机译:大鼠肾上腺培养的肾小球细胞中钙电流的三个成分。

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摘要

1. Ca2+ channels were studied in cultured glomerulosa cells from the rat adrenal gland. The whole-cell configuration of the patch-clamp technique was used. Cs+-filled pipettes were used in order to block K+ channels. 2. Three Ca2+ components were found, namely, T, L and N, according to the nomenclature proposed by Nowycky, Fox & Tsien (1985). The T-component was a fast transient component activated in the range -60 to -40 mV; the L-component did not inactivate for a sustained depolarization and activated at voltages around -30 mV; the third component, the N-component, was transient and was activated at voltages close to -20 mV. 3. A statistical analysis made on seventy-one experiments showed that the L-component was the most frequent (65% of the experiments), followed by the T- and finally the N- components (59 and 29% of the experiments, respectively). 4. The substitution of Ba2+ ions for Ca2+ ions greatly enhanced the L-component's amplitude (iBa/iCa = 4) while the N-component was unaffected and the T-component was reduced (iBa/iCa = 0.4). 5. A comparison of the voltage-dependent steady-state inactivation of the three components showed that the T-component was inactivated at -60 mV while the inactivation of the L- and N-components was complete at -25 and 0 mV, respectively. 6. A run-down effect was detected in some cells. The time stability of the L-component was lower than that of the T-component. The N-component seemed to be insensitive for at least 1 h. The results for the L- and T-components were obtained in cells which presented no run-down of the current or only a weak one. 7. Cd2+ ions (5 x 10(-5)M) completely blocked the long-lasting component (L-component) and slightly decreased the T-component. 8. Bay K 8644, a dihydropyridine agonist, enhanced the L-component at a concentration of 2.5 microM but decreased it for a higher concentration (5 microM). The T-component was decreased in a reversible way by 1 microM-Bay K 8644. Nifedipine, a well-known antagonist, blocked completely the L-component. This effect was reversed by the addition of Bay K 8644 to the perfusion medium. The T-component was also blocked by nifedipine, a result which is in keeping with the fact that Bay K 8644 has a weak effect on this current.
机译:1.在大鼠肾上腺培养的肾小球细胞中研究了Ca2 +通道。使用膜片钳技术的全细胞配置。使用Cs +填充的移液器来阻断K +通道。 2.根据Nowycky,Fox和Tsien(1985)提出的命名法,发现了三个Ca2 +组分,即T,L和N。 T分量是在-60至-40 mV范围内激活的快速瞬态分量; L组分不会因持续去极化而失活,并在-30 mV左右的电压下被激活。第三个成分N成分是瞬态的,并在接近-20 mV的电压下被激活。 3.对71个实验进行的统计分析表明,L分量是最频繁的(实验的65%),其次是T分量,最后是N分量(分别为实验的59%和29%) )。 4.用Ba2 +离子代替Ca2 +离子大大提高了L组分的振幅(iBa / iCa = 4),而N组分未受影响,T组分降低了(iBa / iCa = 0.4)。 5.比较三种成分的电压依赖性稳态失活表明,T成分在-60 mV时失活,而L成分和N成分的失活分别在-25 mV和0 mV时完成。 。 6.在某些细胞中检测到了衰落效应。 L-组分的时间稳定性低于T-组分的时间稳定性。 N组分似乎至少1小时不敏感。 L和T成分的结果是在没有电流损耗或只有很弱电流的电池中获得的。 7. Cd2 +离子(5 x 10(-5)M)完全阻断了持久成分(L成分),并略微降低了T成分。 8. Bay K 8644,一种二氢吡啶激动剂,在2.5 microM的浓度下增强了L成分,但在更高的浓度(5 microM)下降低了L-成分。 1 microM-Bay K 8644以可逆的方式降低了T组分。众所周知的拮抗剂硝苯地平完全阻断了L组分。通过向灌注培养基中添加Bay K 8644可以逆转这种效果。 T组分也被硝苯地平阻断,这一结果与Bay K 8644对这种电流的作用微弱的事实相吻合。

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