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细胞增殖、钙离子内流和钙离子通道。

Cell proliferation, calcium influx and calcium channels.

机构信息

INSERM U807, Faculté de Médecine, 156 rue de Vaugirard, Paris, France.

出版信息

Biochimie. 2011 Dec;93(12):2075-9. doi: 10.1016/j.biochi.2011.07.015. Epub 2011 Jul 23.

Abstract

Both increases in the basal cytosolic calcium concentration (Ca(2+)) and Ca(2+) transients play major roles in cell cycle progression, cell proliferation and division. Calcium transients are observed at various stages of cell cycle and more specifically during late G(1) phase, before and during mitosis. These calcium transients are mainly due to calcium release and reuptake by the endoplasmic reticulum (ER) and are observed over periods of hours in oocytes and mammalian cells. Calcium entry sustains the ER Ca(2+) load and thereby helps to maintain these calcium transients for such a long period. Calcium influx also controls cell growth and proliferation in several cell types. Various calcium channels are involved in this process and the tight relation between the expression and activity of cyclins and calcium channels also suggests that calcium entry may be needed only at particular stages of the cell cycle. Consistent with this idea, the expression of l-type and T-type calcium channels and SOCE amplitude fluctuate along the cell cycle. But, as calcium influx regulates several other transduction pathways, the presence of a specific connection to trigger activation of proliferation and cell division in mammalian cells will be discussed in this review.

摘要

基础细胞质钙离子浓度(Ca(2+))和Ca(2+)瞬变的增加都在细胞周期进程、细胞增殖和分裂中发挥主要作用。钙离子瞬变发生在细胞周期的各个阶段,更具体地说,在晚期 G1 期、有丝分裂前期和有丝分裂期间观察到钙离子瞬变。这些钙离子瞬变主要是由于内质网(ER)的钙离子释放和再摄取引起的,在卵母细胞和哺乳动物细胞中可以观察到数小时的周期。钙离子内流维持 ER 钙离子负荷,从而有助于维持如此长的钙离子瞬变。钙离子内流还控制着几种细胞类型的细胞生长和增殖。各种钙通道参与了这个过程,而且细胞周期蛋白和钙通道的表达和活性之间的紧密关系也表明,钙离子内流可能仅在细胞周期的特定阶段才是必需的。与这一观点一致的是,L 型和 T 型钙通道的表达和 SOCE 幅度沿细胞周期波动。但是,由于钙离子内流调节着其他几个信号转导途径,因此在本文综述中,将讨论在哺乳动物细胞中触发增殖和细胞分裂激活的特定连接的存在。

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