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Neuronal cdc2-like kinase: a cdc2-related protein kinase with predominantly neuronal expression.

机译:神经元cdc2样激酶:与cdc2相关的蛋白激酶主要表达神经元。

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摘要

Recent studies have shown that there exists a family of protein kinases structurally and functionally related to the yeast cell cycle regulatory kinase cdc2 [Meyerson, M., Faha, B., Su, L.-K., Harlow, E. & Tsai, L.-H. (1991) Cold Spring Harbor Symp. Quant. Biol. 56, 177-186 and Meyerson, M., Enders, G. H., Wu, C.-L., Su, L.-K., Gorka, C., Nelson, C., Harlow, E. & Tsai, L.-H. (1992) EMBO J. 11, 2909-2917]. Two members of cdc2 family, p34cdc2 (also named cdk1) and cdk2, have been identified in mammalian cells. cdk1 kinase regulates the progression from G2 to M phase, and cdk2 kinase has been proposed to regulate the progression from G1 to S phase. In this work, we have cloned and structurally characterized a third member of the cdc2 kinase family with 58% amino acid sequence identity to mouse cdk1 and 61% identity to human cdk2. We call this kinase neuronal cdc2-like kinase (nclk) because, in contrast to either cdk1 or cdk2, nclk is expressed at high levels in terminally differentiated neurons no longer in the cell cycle. Previous studies have shown [Hisanaga, S., Kusubata, M., Okumura, E. & Kishimoto, T. (1991) J. Biol. Chem. 266, 21798-21803 and Guan, R. J., Hall, F. L. & Cohlberg, J. A. (1992) J. Neurochem. 58, 1365-1371] that cdk1 kinase, but not other structurally defined protein kinases, could phosphorylate the repeated Lys-Ser-Pro (KSP) motifs found in mammalian high and middle molecular mass neurofilament subunits in vitro, but the precise molecular nature of the endogenous neuronal KSP kinase has remained undefined. The structural similarity of nclk to cdk1 kinase and its high level of expression in terminally differentiated neurons suggest that nclk may play a role in the phosphorylation of the neurofilament KSP repeats in vivo, a function distinct from cell cycle regulation.
机译:最近的研究表明,存在与酵母细胞周期调节激酶cdc2在结构和功能上相关的蛋白激酶家族[Meyerson,M.,Faha,B.,Su,L.-K.,Harlow,E.&Tsai, L.-H. (1991)冷泉港症状。数量生物学56,177-186和Meyerson,M.,Enders,GH,Wu,C.-L.,Su,L.-K.,Gorka,C.,Nelson,C.,Harlow,E.&Tsai,L. -H。 (1992)EMBO J. 11,2909-2917]。在哺乳动物细胞中已鉴定出cdc2家族的两个成员p34cdc2(也称为cdk1)和cdk2。 cdk1激酶调节从G2到M期的进程,有人提出cdk2激酶调节从G1到S期的进程。在这项工作中,我们克隆了cdc2激酶家族的第三个成员,并在结构上鉴定了其与小鼠cdk1的氨基酸序列同源性为58%,与人cdk2的氨基酸序列同源性为61%。我们将这种激酶称为神经元cdc2样激酶(nclk),因为与cdk1或cdk2相比,nclk在不再处于细胞周期的终末分化神经元中高水平表达。先前的研究已经显示[Hisagaga,S.,Kusubata,M.,Okumura,E。和Kishimoto,T。(1991)J.Biol.Chem.Soc。,1992。化学266,21798-21803和Guan,R.J.,Hall,F.L.&Cohlberg,J.A.(1992)J.Neurochem。 58,1365-1371]指出cdk1激酶可磷酸化在哺乳动物高中分子神经丝亚单位中发现的重复Lys-Ser-Pro(KSP)基序,但其结构的确切分子性质却不能磷酸化磷酸化。内源性神经元KSP激酶尚未确定。 nclk与cdk1激酶的结构相似性及其在终末分化神经元中的高表达水平表明nclk可能在体内神经丝KSP重复序列的磷酸化中起作用,其功能不同于细胞周期调控。

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