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组胺H1受体激活诱导间期和有丝分裂期HeLa细胞内游离钙升高:激素信号转导在有丝分裂期间发生改变。

Intracellular elevations of free calcium induced by activation of histamine H1 receptors in interphase and mitotic HeLa cells: hormone signal transduction is altered during mitosis.

作者信息

Volpi M, Berlin R D

机构信息

Department of Physiology, University of Connecticut Health Center, Farmington 06032.

出版信息

J Cell Biol. 1988 Dec;107(6 Pt 2):2533-9. doi: 10.1083/jcb.107.6.2533.

Abstract

A broad range of membrane functions, including endocytosis and exocytosis, are strongly inhibited during mitosis. The underlying mechanisms are unclear, however, but will probably be important in relation to the mitotic cycle and the regulation of surface phenomena generally. A major unanswered question is whether membrane signal transduction is altered during mitosis; suppression of an intracellular calcium [( Ca2+]i) transient could inhibit exocytosis; [Ca2+]i elevation could disassemble the mitotic spindle. Activation of the histamine H1 receptor interphase in HeLa cells is shown here by Indo-1 fluorescence to produce a transient elevation of [Ca2+]i. The [Ca2+]i transient consists of an initial sharp rise that is at least partially dependent on intracellular calcium followed by an elevated plateau that is absolutely dependent on extracellular calcium. The [Ca2+]i transient is completely suppressed by preincubation with the tumor promoter, phorbol myristate acetate, but is unaffected by preincubation with pertussis toxin (islet-activating protein). In mitotic (metaphase-arrested) HeLa cells, the [Ca2+]i transient is largely limited to the initial peak. Measurement of 45Ca2+ uptake shows that it is stimulated by histamine in interphase cells, but not in mitotics. We conclude that the histamine-stimulated generation of the second messenger, [Ca2+]i, in mitotic cells is limited by failure to activate a sustained calcium influx. The initial phase of calcium mobilization from intracellular stores is comparable to that in interphase cells. Hormone signal transduction thus appears to be altered during mitosis.

摘要

包括胞吞作用和胞吐作用在内的多种膜功能在有丝分裂期间受到强烈抑制。然而,其潜在机制尚不清楚,但可能与有丝分裂周期以及一般表面现象的调节密切相关。一个主要未解决的问题是膜信号转导在有丝分裂期间是否发生改变;细胞内钙瞬变的抑制可能会抑制胞吐作用;细胞内钙升高可能会使有丝分裂纺锤体解体。本文通过Indo-1荧光显示,组胺H1受体在HeLa细胞间期的激活会导致细胞内钙瞬变升高。细胞内钙瞬变包括一个初始的急剧上升,这至少部分依赖于细胞内钙,随后是一个绝对依赖于细胞外钙的升高平台期。细胞内钙瞬变通过与肿瘤启动子佛波醇肉豆蔻酸酯预孵育而被完全抑制,但与百日咳毒素(胰岛激活蛋白)预孵育则不受影响。在有丝分裂(中期阻滞)的HeLa细胞中,细胞内钙瞬变主要局限于初始峰值。45Ca2+摄取的测量表明,组胺在间期细胞中能刺激其摄取,但在有丝分裂细胞中则不能。我们得出结论,在有丝分裂细胞中,组胺刺激产生的第二信使细胞内钙,因未能激活持续的钙内流而受到限制。从细胞内储存库动员钙的初始阶段与间期细胞中的情况相当。因此,激素信号转导在有丝分裂期间似乎发生了改变。

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