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在脱离失能状态恢复过程中分离的大鼠肝细胞内短暂的45Ca摄取与释放

Transient 45Ca uptake and release in isolated rat-liver cells during recovery from deenergized states.

作者信息

Krell H, Baur H, Pfaff E

出版信息

Eur J Biochem. 1979 Nov;101(2):349-64. doi: 10.1111/j.1432-1033.1979.tb19727.x.

Abstract
  1. Aerobic incubation of isolated rat liver cells--after dilution from the anaerobic stock suspension--transiently brings about a state, during which a reversible calcium uptake can be observed on addition of a respiratory substrate. Uptake varies greatly and can reach more than 50 nmol/mg protein, but declines to zero on prolonged preincubation, especially at higher temperature. Repeated additions of succinate or 3-hydroxybutyrate evoke new calcium transients. If ATP is simultaneously added, if greatly potentiates succinate-initiated reversible uptake. 2. If rotenone is present during the preincubation phase, calcium transients are strongly enhanced. Uptake is blocked by uncouplers and respiratory inhibitors, indicating the involvement of mitochondria. 3. Calcium uptake is not accompanied by increased oxygen consumption. The actual respiration cannot account sufficiently for the energy need of calcium uptake. Participation of cytoplasmic ATP is likely, as inhibitors of adenine nucleotide translocase affect uptake. 4. Lanthanum enhances calcium uptake in contrast to its action on mitochondria. 5. Pulse-labeling experiments indicate that the calcium taken up is removed from a rapidly exchangeable calcium pool by withdrawal into the mitochondria as a deep compartment. 6. Calcium uptake is accelerated either by increasing the phosphate level or by high temperature. It is prolonged by low temperature, high pH or high ATP concentration. Calcium release accelerates with increasing temperature, decreasing pH and a further rise in phosphate concentration. 7. The dependency on phosphate and temperature reveals a delicately poised equilibrium of uptake and release. At ambient temperature, phosphate increases uptake up to a concentration of 0.5 mM. Higher concentrations accelerate both uptake and release. At lower temperature, the accelerating effect on uptake predominates. A temperature shift during incubation results in adaptation of the calcium equilibrium to the new temperature, i.e. release of calcium at high temperature, uptake at low temperature. 8. Oxidizing metabolites inhibit succinate-stimulated calcium uptake and promote release of previously accumulated calcium. An increased sensitivity to phosphate is established. 9. With respect to isolated mitochondria, isolated liver cells appear to be a more realistic model for studying the physiological mechanism of mitochondrial calcium release, since compartmental constraints and regulations are maintained.
摘要
  1. 分离的大鼠肝细胞经厌氧储备悬液稀释后进行需氧孵育,会短暂出现一种状态,在此期间,添加呼吸底物后可观察到可逆的钙摄取。摄取量变化很大,可达50 nmol/mg蛋白质以上,但长时间预孵育后会降至零,尤其是在较高温度下。重复添加琥珀酸盐或3-羟基丁酸盐会引发新的钙瞬变。如果同时添加ATP,则会极大地增强琥珀酸盐引发的可逆摄取。2. 如果在预孵育阶段存在鱼藤酮,钙瞬变会显著增强。摄取会被解偶联剂和呼吸抑制剂阻断,表明线粒体参与其中。3. 钙摄取并不伴随着氧消耗的增加。实际的呼吸作用不足以充分满足钙摄取的能量需求。细胞质ATP可能参与其中,因为腺嘌呤核苷酸转位酶抑制剂会影响摄取。4. 与镧对线粒体的作用相反,镧会增强钙摄取。5. 脉冲标记实验表明,摄取的钙通过进入线粒体这一深层区室而从快速可交换钙池中被移除。6. 通过提高磷酸盐水平或高温可加速钙摄取。低温、高pH值或高ATP浓度会延长钙摄取时间。随着温度升高、pH值降低以及磷酸盐浓度进一步升高,钙释放会加速。7. 对磷酸盐和温度的依赖性揭示了摄取和释放之间微妙平衡的状态。在环境温度下,磷酸盐会使摄取量增加,直至浓度达到0.5 mM。更高的浓度会加速摄取和释放。在较低温度下,对摄取的加速作用占主导。孵育过程中的温度变化会导致钙平衡适应新温度,即在高温下释放钙,在低温下摄取钙。8. 氧化代谢物会抑制琥珀酸盐刺激的钙摄取,并促进先前积累的钙的释放。对磷酸盐的敏感性增加。9. 就分离的线粒体而言,分离的肝细胞似乎是研究线粒体钙释放生理机制的更现实模型,因为其区室限制和调节得以维持。

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