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海胆卵有丝分裂过程中组蛋白H1激酶的周期性激活。

Cyclic activation of histone H1 kinase during sea urchin egg mitotic divisions.

作者信息

Meijer L, Pondaven P

机构信息

Station Biologique, Roscoff, France.

出版信息

Exp Cell Res. 1988 Jan;174(1):116-29. doi: 10.1016/0014-4827(88)90147-4.

Abstract

Fertilized sea urchin eggs undergo a series of rapid and synchronized mitotic divisions. Extracts were made at various times throughout the first three mitotic divisions and assayed for phosphorylating activity toward histone H1. Histone H1 kinase (HH1K) undergoes a transient activation (8- to 10-fold increase) 20 min before each cleavage. The amplitude of the HH1K peak strongly depends on the synchrony of the egg population. Concomitant cytological observations show that the time-course of HH1K correlates with the time-course of nuclear envelope breakdown and of metaphase. This correlation is observed at each cell division cycle. HH1K from each of the three first mitoses show identical time- and concentration-dependence curves as well as identical dose-inhibition curves with 6-dimethylaminopurine and quercetin, suggesting that the same (group of) kinase(s) is (are) activated before each cleavage. Ionophore A23187 does not trigger, but inhibits, HH1K activation; however, partial activation of the eggs with ammonia at pH 9.0 (but not at pH 8.0) triggers the transient HH1K activation. Appearance of the HH1K cycle requires protein synthesis since it is completely abolished in emetine-treated eggs. Although cytochalasin B blocks egg cleavage, it does not inhibit HH1K activation nor nuclear divisions. A prolonged HH1K activation cycle is observed in eggs arrested in metaphase with colchicine or nocodazole. Despite the existence of a cycle in cAMP concentration during mitosis, forskolin, an activator of adenylate cyclase, does not modify the time-course of HH1K activation and of cell division. The cycling HH1K is independent of calcium-calmodulin, calcium-phospholipids, or cyclic AMP. It clearly resembles the mammalian "growth-associated histone kinase." The relationship between the transient activation of HH1K and the intracellular mitotic factors driving the cell cycle is discussed.

摘要

受精的海胆卵会经历一系列快速且同步的有丝分裂。在最初的三次有丝分裂的不同时间点制备提取物,并检测其对组蛋白H1的磷酸化活性。组蛋白H1激酶(HH1K)在每次卵裂前20分钟会经历短暂激活(增加8至10倍)。HH1K峰值的幅度强烈依赖于卵群体的同步性。同时进行的细胞学观察表明,HH1K的时间进程与核膜破裂和中期的时间进程相关。在每个细胞分裂周期中都观察到这种相关性。来自前三次有丝分裂中每次的HH1K显示出相同的时间和浓度依赖性曲线,以及与6 - 二甲基氨基嘌呤和槲皮素相同的剂量抑制曲线,这表明在每次卵裂前激活的是相同的(一组)激酶。离子载体A23187不会触发而是抑制HH1K的激活;然而,在pH 9.0(而非pH 8.0)下用氨对卵进行部分激活会触发HH1K的短暂激活。HH1K循环的出现需要蛋白质合成,因为在用依米丁处理的卵中它会完全消失。尽管细胞松弛素B会阻断卵裂,但它并不抑制HH1K的激活或核分裂。在用秋水仙碱或诺考达唑使卵阻滞在中期时,会观察到HH1K激活周期延长。尽管在有丝分裂期间cAMP浓度存在循环,但腺苷酸环化酶的激活剂福斯高林并不会改变HH1K激活和细胞分裂的时间进程。循环中的HH1K独立于钙 - 钙调蛋白、钙 - 磷脂或环磷酸腺苷。它明显类似于哺乳动物的“生长相关组蛋白激酶”。文中讨论了HH1K的短暂激活与驱动细胞周期的细胞内有丝分裂因子之间的关系。

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