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酵母中心体蛋白的细胞周期依赖性磷酸化调节γ-TuSC介导的微管成核。

Cell-cycle dependent phosphorylation of yeast pericentrin regulates γ-TuSC-mediated microtubule nucleation.

作者信息

Lin Tien-Chen, Neuner Annett, Schlosser Yvonne T, Scharf Annette N D, Weber Lisa, Schiebel Elmar

机构信息

Zentrum für Molekulare Biologie (ZMBH), Universität Heidelberg, Heidelberg, Germany The Hartmut Hoffmann-Berling International Graduate School, University of Heidelberg, Heidelberg, Germany.

Zentrum für Molekulare Biologie (ZMBH), Universität Heidelberg, Heidelberg, Germany.

出版信息

Elife. 2014 Apr 30;3:e02208. doi: 10.7554/eLife.02208.

Abstract

Budding yeast Spc110, a member of γ-tubulin complex receptor family (γ-TuCR), recruits γ-tubulin complexes to microtubule (MT) organizing centers (MTOCs). Biochemical studies suggest that Spc110 facilitates higher-order γ-tubulin complex assembly (Kollman et al., 2010). Nevertheless the molecular basis for this activity and the regulation are unclear. Here we show that Spc110 phosphorylated by Mps1 and Cdk1 activates γ-TuSC oligomerization and MT nucleation in a cell cycle dependent manner. Interaction between the N-terminus of the γ-TuSC subunit Spc98 and Spc110 is important for this activity. Besides the conserved CM1 motif in γ-TuCRs (Sawin et al., 2004), a second motif that we named Spc110/Pcp1 motif (SPM) is also important for MT nucleation. The activating Mps1 and Cdk1 sites lie between SPM and CM1 motifs. Most organisms have both SPM-CM1 (Spc110/Pcp1/PCNT) and CM1-only (Spc72/Mto1/Cnn/CDK5RAP2/myomegalin) types of γ-TuCRs. The two types of γ-TuCRs contain distinct but conserved C-terminal MTOC targeting domains.DOI: http://dx.doi.org/10.7554/eLife.02208.001.

摘要

出芽酵母的Spc110是γ-微管蛋白复合体受体家族(γ-TuCR)的成员之一,可将γ-微管蛋白复合体招募至微管(MT)组织中心(MTOC)。生化研究表明,Spc110促进了高阶γ-微管蛋白复合体的组装(Kollman等人,2010年)。然而,这种活性及其调控的分子基础尚不清楚。在此我们表明,由Mps1和Cdk1磷酸化的Spc110以细胞周期依赖性方式激活γ-TuSC寡聚化和MT成核。γ-TuSC亚基Spc98的N端与Spc110之间的相互作用对该活性很重要。除了γ-TuCRs中保守的CM1基序(Sawin等人,2004年)外,我们命名为Spc110/Pcp1基序(SPM)的第二个基序对MT成核也很重要。激活的Mps1和Cdk1位点位于SPM和CM1基序之间。大多数生物体都有SPM-CM1(Spc110/Pcp1/PCNT)和仅含CM1(Spc72/Mto1/Cnn/CDK5RAP2/巨肌蛋白)这两种类型的γ-TuCRs。这两种类型的γ-TuCRs包含不同但保守的C端MTOC靶向结构域。DOI: http://dx.doi.org/10.7554/eLife.02208.001

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6816/4034690/52fbbace943e/elife02208f002.jpg

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