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三种相互作用的正端追踪蛋白对酿酒酵母微管动力学的调控

The regulation of microtubule dynamics in Saccharomyces cerevisiae by three interacting plus-end tracking proteins.

作者信息

Wolyniak Michael J, Blake-Hodek Kristina, Kosco Karena, Hwang Eric, You Liru, Huffaker Tim C

机构信息

Department of Molecular Biology and Genetics, Cornell University, Ithaca, NY 14853-2703, USA.

出版信息

Mol Biol Cell. 2006 Jun;17(6):2789-98. doi: 10.1091/mbc.e05-09-0892. Epub 2006 Mar 29.

Abstract

Microtubule plus-end tracking proteins (+TIPs) are a diverse group of molecules that regulate microtubule dynamics and interactions of microtubules with other cellular structures. Many +TIPs have affinity for each other but the functional significance of these associations is unclear. Here we investigate the physical and functional interactions among three +TIPs in S. cerevisiae, Stu2, Bik1, and Bim1. Two-hybrid, coimmunoprecipitation, and in vitro binding assays demonstrate that they associate in all pairwise combinations, although the interaction between Stu2 and Bim1 may be indirect. Three-hybrid assays indicate that these proteins compete for binding to each other. Thus, Stu2, Bik1, and Bim1 interact physically but do not appear to be arranged in a single unique complex. We examined the functional interactions among pairs of proteins by comparing cytoplasmic and spindle microtubule dynamics in cells lacking either one or both proteins. On cytoplasmic microtubules, Stu2 and Bim1 act cooperatively to regulate dynamics in G1 but not in preanaphase, whereas Bik1 acts independently from Stu2 and Bim1. On kinetochore microtubules, Bik1 and Bim1 are redundant for regulating dynamics, whereas Stu2 acts independently from Bik1 and Bim1. These results indicate that interactions among +TIPS can play important roles in the regulation of microtubule dynamics.

摘要

微管正端追踪蛋白(+TIPs)是一类多样的分子,它们调节微管动力学以及微管与其他细胞结构的相互作用。许多+TIPs彼此之间具有亲和力,但这些关联的功能意义尚不清楚。在这里,我们研究了酿酒酵母中三种+TIPs,即Stu2、Bik1和Bim1之间的物理和功能相互作用。双杂交、共免疫沉淀和体外结合试验表明,它们以所有两两组合的方式相互关联,尽管Stu2和Bim1之间的相互作用可能是间接的。三杂交试验表明这些蛋白质相互竞争结合。因此,Stu2、Bik1和Bim1在物理上相互作用,但似乎并没有形成单一独特的复合物。我们通过比较缺乏其中一种或两种蛋白质的细胞中细胞质和纺锤体微管的动力学,研究了蛋白质对之间的功能相互作用。在细胞质微管上,Stu2和Bim1协同作用以调节G1期的动力学,但在后期前则不然,而Bik1独立于Stu2和Bim1发挥作用。在动粒微管上,Bik1和Bim1在调节动力学方面是冗余的,而Stu2独立于Bik1和Bim1发挥作用。这些结果表明,+TIPs之间的相互作用在微管动力学调节中可能发挥重要作用。

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