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肌浆网Ca(2+)-ATP酶抑制剂环匹阿尼酸对豚鼠离体心房收缩-舒张周期频率依赖性的影响。

Effect of cyclopiazonic acid, an inhibitor of sarcoplasmic reticulum Ca(2+)-ATPase, on the frequency-dependence of the contraction-relaxation cycle of the guinea-pig isolated atrium.

作者信息

Yard N J, Chiesi M, Ball H A

机构信息

Cardiovascular Biology Research Department, Ciba-Geigy Ltd., Basel, Switzerland.

出版信息

Br J Pharmacol. 1994 Nov;113(3):1001-7. doi: 10.1111/j.1476-5381.1994.tb17092.x.

Abstract
  1. The relevance of a functional sarcoplasmic reticulum (SR) membrane system to the contraction-relaxation cycle and to the force-frequency relationship of guinea-pig atrial tissue was investigated. Cyclopiazonic acid (CPA) was used to inhibit selectively the activity of the SR Ca(2+)-ATPase. IC50 values of 0.2 microM or 1.0 microM were measured in guinea-pig isolated SR membranes in the absence or presence of millimolar ATP, respectively. CPA (0.3-30 microM) did not inhibit the activity of the sarcolemmal Na(+)-Ca(2+)-exchanger as measured in isolated cardiac cell membrane preparations. 2. In guinea-pig isolated left atrium paced at 2.5 Hz (30 degrees C), CPA (1-100 microM) produced a concentration-dependent reduction in developed tension and a fall in the maximum rate of tension increase (+dT/dtmax) and decrease (-dT/dtmax). The twitch duration was markedly increased due to a prolongation of the time to peak tension, and in particular, the relaxation phase. 3. The contraction-relaxation cycle of the left atrium showed a marked dependence on the frequency of stimulation. The developed tension and +dT/dtmax showed a progressive increase from 0.5 Hz, reaching peak values at a stimulation rate of 1.5-2.5 Hz, the positive staircase phenomenon. Higher frequencies of stimulation caused a fall in these parameters. Resting tension was unaffected. The time-course of the contraction-relaxation cycle was also frequency-dependent, with both time to peak tension and relaxation time showing a progressive fall from 2.0-3.5 Hz. 4. The addition of CPA (30 microM) caused marked alterations in the frequency-dependence of the contraction-relaxation cycle. The frequency-dependence of developed tension, + dr/dtmax and dT/dt max was shifted downwards, particularly at higher frequencies, and the frequency at which peak values of+ dT/dtmax and - dT/dtmax were reached was shifted leftwards. The resting tension of the tissues in the presence of 30 micro M CPA was increased markedly at frequencies greater than 2 Hz. The time-course of the contraction-relaxation cycle was markedly prolonged between 1.0 and 3.5 Hz, due to an effect on both time to peak tension and relaxation time.5. In conclusion, these results show that CPA is a highly selective inhibitor of the cardiac SR Ca2+-ATPase, without effect on the sarcolemmal Na+-Ca2+-exchanger, and suggest that a functional SR Ca2+-ATPase is necessary for the normal contraction-relaxation cycle of guinea-pig cardiac tissue.Additionally, the results suggest an increasing dependence of tension development on SR Ca2+-ATPase with increasing frequency, which may reflect either a frequency-dependent activation of this enzyme or the diminished contribution of the Na+-Ca2+ exchanger. These results also provide novel support for the mechanism of the depressed force-frequency relation found in cardiac tissue of heart failure patients, in which there is a reduced expression of Ca2+-ATPase.
摘要
  1. 研究了功能性肌浆网(SR)膜系统与豚鼠心房组织收缩 - 舒张周期以及力 - 频率关系的相关性。用环匹阿尼酸(CPA)选择性抑制SR Ca²⁺ - ATP酶的活性。在不存在或存在毫摩尔ATP的情况下,分别在豚鼠分离的SR膜中测得IC50值为0.2微摩尔或1.0微摩尔。在分离的心肌细胞膜制剂中测得,CPA(0.3 - 30微摩尔)不抑制肌膜钠 - 钙交换体的活性。2. 在30℃以2.5 Hz起搏的豚鼠离体左心房中,CPA(1 - 100微摩尔)使舒张期张力呈浓度依赖性降低,张力增加的最大速率(+dT/dtmax)下降以及张力降低速率(-dT/dtmax)下降。由于达到峰值张力的时间延长,特别是舒张期延长,收缩期持续时间显著增加。3. 左心房的收缩 - 舒张周期对刺激频率有明显依赖性。舒张期张力和 +dT/dtmax从0.5 Hz开始逐渐增加,在刺激频率为1.5 - 2.5 Hz时达到峰值,即正阶梯现象。更高的刺激频率导致这些参数下降。静息张力不受影响。收缩 - 舒张周期的时间进程也与频率有关,达到峰值张力的时间和舒张时间从2.0 - 3.5 Hz都逐渐下降。4. 添加CPA(30微摩尔)导致收缩 - 舒张周期的频率依赖性发生明显改变。舒张期张力、+ dr/dtmax和dT/dt max的频率依赖性向下移动,特别是在较高频率时,并且达到 +dT/dtmax和 -dT/dtmax峰值的频率向左移动。在频率大于2 Hz时,存在30微摩尔CPA的组织的静息张力显著增加。在1.0至3.5 Hz之间,收缩 - 舒张周期的时间进程显著延长,这是由于对达到峰值张力的时间和舒张时间都有影响。5. 总之,这些结果表明CPA是心脏SR Ca²⁺ - ATP酶的高度选择性抑制剂,对肌膜钠 - 钙交换体无影响,并表明功能性SR Ca²⁺ - ATP酶是豚鼠心脏组织正常收缩 - 舒张周期所必需的。此外,结果表明随着频率增加,张力发展对SR Ca²⁺ - ATP酶的依赖性增加,这可能反映了该酶的频率依赖性激活或钠 - 钙交换体贡献的减少。这些结果也为心力衰竭患者心脏组织中发现的力 - 频率关系降低的机制提供了新的支持,其中Ca²⁺ - ATP酶的表达减少。

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