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Slk19 增强了 Ase1 和 Stu1 对微管的交联。

Slk19 enhances cross-linking of microtubules by Ase1 and Stu1.

机构信息

Biochemie-Zentrum der Universität Heidelberg, INF 328, 69120 Heidelberg, Germany.

出版信息

Mol Biol Cell. 2021 Nov 1;32(21):ar22. doi: 10.1091/mbc.E21-05-0279. Epub 2021 Sep 8.

Abstract

The protein Slk19 has been shown to localize to kinetochores throughout mitosis and to the spindle midzone in anaphase. However, Slk19 clearly also has an important role for spindle formation and stabilization in prometaphase and metaphase, albeit this role is unresolved. Here we show that Slk19's localization to metaphase spindles in vivo and to microtubules (MTs) in vitro depends on the MT cross-linking protein Ase1 and the MT cross-linking and stabilizing protein Stu1. By analyzing a mutant that specifically fails to localize to spindles and MTs, we surprisingly found that the presence of Slk19 amplified the amount of Ase1 strongly and that of Stu1 moderately at the metaphase spindle in vivo and at MTs in vitro. Furthermore, Slk19 markedly enhanced the cross-linking of MTs in vitro when added together with Ase1 or Stu1. We therefore suggest that Slk19 recruits additional Ase1 and Stu1 to the interpolar MTs (ipMTs) of metaphase spindles and thus increases their cross-linking and stabilization. This is in agreement with our observation that cells with defective Slk19 localization exhibit shorter metaphase spindles, an increased number of unaligned nuclear MTs, and most likely reduced ipMT overlaps.

摘要

Slk19 蛋白已被证明在整个有丝分裂过程中定位于动粒,在后期定位于纺锤体中部。然而,Slk19 显然在前期和中期对纺锤体的形成和稳定也有重要作用,尽管其作用尚未得到解决。在这里,我们表明 Slk19 在体内定位于中期纺锤体和体外定位于微管(MTs)依赖于 MT 交联蛋白 Ase1 和 MT 交联和稳定蛋白 Stu1。通过分析一种特异性不能定位到纺锤体和 MTs 的突变体,我们惊讶地发现,Slk19 的存在强烈地增加了体内中期纺锤体和体外 MTs 中 Ase1 的数量,并适度地增加了 Stu1 的数量。此外,Slk19 与 Ase1 或 Stu1 一起添加时,显著增强了 MTs 在体外的交联。因此,我们认为 Slk19 将额外的 Ase1 和 Stu1 募集到中期纺锤体的两极 MTs(ipMTs),从而增加它们的交联和稳定性。这与我们的观察结果一致,即 Slk19 定位缺陷的细胞表现出较短的中期纺锤体、未对齐的核 MTs 数量增加,并且很可能降低了 ipMT 重叠。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/82d1/8693956/438457b87546/mbc-32-ar22-g001.jpg

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