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Genetic and biochemical interactions between an essential kinetochore protein Cbf2p/Ndc10p and the CDC34 ubiquitin-conjugating enzyme.

机译:基本的线粒体蛋白Cbf2p / Ndc10p和CDC34泛素结合酶之间的遗传和生化相互作用。

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摘要

CBF2/NDC10/CTF14 encodes the 110-kDa subunit of CBF3, a key component of the yeast centromere/kinetochore. Overexpression of yeast CDC34 specifically suppresses the temperature-sensitive growth phenotype of the ndc10-1 mutation. Mutations in CDC34, which specifies a ubiquitin-conjugating enzyme, arrest yeast cells in the G1 phase of the cell cycle, with no intact spindles formed (M. G. Goebl, J. Yochem, S. Jentsch, J. P. McGrath, A. Varshavsky, and B. Byers, Science 241:1331-1335, 1988). The cdc34-2 mutation drastically alters the pattern of Cbf2p modification. Results of experiments using antibodies against Cbf2p and ubiquitin indicate that Cbf2p is ubiquitinated in vivo. Purified Cdc34p catalyzes the formation of Cbf2p-monoubiquitin conjugate in vitro. These data suggest that Cbf2p is an endogenous substrate of the CDC34 ubiquitin-conjugating enzyme and imply that ubiquitination of a kinetochore protein plays a regulatory role in kinetochore function.
机译:CBF2 / NDC10 / CTF14编码CBF3的110-kDa亚基,CBF3是酵母着丝粒/动粒的关键成分。酵母CDC34的过度表达可特异性抑制ndc10-1突变的温度敏感型生长表型。 CDC34中的突变指定了泛素结合酶,使酵母细胞停滞在细胞周期的G1期,没有形成完整的纺锤体(MG Goebl,J。Yochem,S。Jentsch,JP McGrath,A。Varshavsky和B (Byers,Science 241:1331-1335,1988)。 cdc34-2突变大大改变了Cbf2p修饰的模式。使用针对Cbf2p和泛素的抗体的实验结果表明,Cbf2p在体内被泛素化。纯化的Cdc34p在体外催化Cbf2p-单泛素缀合物的形成。这些数据表明,Cbf2p是CDC34泛素结合酶的内源性底物,暗示着线粒体蛋白的泛素化在线粒体功能中起调节作用。

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