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Spc98p将酵母γ-微管蛋白复合体导入细胞核,并在纺锤体极体的核侧发生细胞周期依赖性磷酸化。

Spc98p directs the yeast gamma-tubulin complex into the nucleus and is subject to cell cycle-dependent phosphorylation on the nuclear side of the spindle pole body.

作者信息

Pereira G, Knop M, Schiebel E

机构信息

Max-Planck Institut für Biochemie, 82152 Martinsried, Germany.

出版信息

Mol Biol Cell. 1998 Apr;9(4):775-93. doi: 10.1091/mbc.9.4.775.

Abstract

In the yeast Saccharomyces cerevisiae, microtubules are organized by the spindle pole body (SPB), which is embedded in the nuclear envelope. Microtubule organization requires the gamma-tubulin complex containing the gamma-tubulin Tub4p, Spc98p, and Spc97p. The Tub4p complex is associated with cytoplasmic and nuclear substructures of the SPB, which organize the cytoplasmic and nuclear microtubules. Here we present evidence that the Tub4p complex assembles in the cytoplasm and then either binds to the cytoplasmic side of the SPB or is imported into the nucleus followed by binding to the nuclear side of the SPB. Nuclear import of the Tub4p complex is mediated by the essential nuclear localization sequence of Spc98p. Our studies also indicate that Spc98p in the Tub4p complex is phosphorylated at the nuclear, but not at the cytoplasmic, side of the SPB. This phosphorylation is cell cycle dependent and occurs after SPB duplication and nucleation of microtubules by the new SPB and therefore may have a role in mitotic spindle function. In addition, activation of the mitotic checkpoint stimulates Spc98p phosphorylation. The kinase Mps1p, which functions in SPB duplication and mitotic checkpoint control, seems to be involved in Spc98p phosphorylation. Our results also suggest that the nuclear and cytoplasmic Tub4p complexes are regulated differently.

摘要

在酿酒酵母中,微管由嵌入核膜的纺锤体极体(SPB)组织形成。微管组织需要包含γ-微管蛋白Tub4p、Spc98p和Spc97p的γ-微管蛋白复合体。Tub4p复合体与SPB的细胞质和核亚结构相关联,这些亚结构组织细胞质和核微管。在此,我们提供证据表明,Tub4p复合体在细胞质中组装,然后要么与SPB的细胞质侧结合,要么被导入细胞核,随后与SPB的核侧结合。Tub4p复合体的核输入由Spc98p的必需核定位序列介导。我们的研究还表明,Tub4p复合体中的Spc98p在SPB的核侧而非细胞质侧被磷酸化。这种磷酸化是细胞周期依赖性的,发生在SPB复制以及新的SPB形成微管核之后,因此可能在有丝分裂纺锤体功能中发挥作用。此外,有丝分裂检查点的激活会刺激Spc98p磷酸化。在SPB复制和有丝分裂检查点控制中起作用的激酶Mps1p似乎参与了Spc98p的磷酸化。我们的结果还表明,核内和胞质中的Tub4p复合体受到不同的调节。

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