Ccl1是一种与蛋白激酶Kin28相关的细胞周期蛋白,控制RNA聚合酶II最大亚基的磷酸化和mRNA转录。

J G Valay, M F Dubois, O Bensaude, G Faye
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引用次数: 0

摘要

Kin28蛋白激酶与细胞周期蛋白Ccl1在物理和遗传上相互作用。最近有报道称,Kin28参与了酿酒酵母RNA聚合酶II (Rpb1)最大亚基的体内磷酸化。现在,我们发现在一个具有条件ccl1-ts突变的菌株中,Rpb1亚基的c端结构域(CTD)在限制性温度下被低磷酸化。随机选择的一组基因的转录在限制性温度下的kin28-ts突变体中受到严重影响。在这里,我们报道了同一组基因需要一个功能性的CCL1基因产物来转录。这些发现,加上先前发表的数据,确定了Kin28p是一种周期蛋白依赖性激酶(CDK), Ccl1p作为伴侣,两者都是一般转录和CTD磷酸化所必需的。
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Ccl1, a cyclin associated with protein kinase Kin28, controls the phosphorylation of RNA polymerase II largest subunit and mRNA transcription.

The Kin28 protein kinase interacts physically and genetically with cyclin Ccl1. Kin28 has been reported recently to be involved in the in vivo phosphorylation of the largest subunit of RNA polymerase II (Rpb1) in Saccharomyces cerevisiae. Now, we show that in a strain harboring a conditional ccl1-ts mutation, the C-terminal domain (CTD) of the Rpb1 subunit is under-phosphorylated at restrictive temperature. The transcription of a set of genes, chosen at random, is severely affected in a kin28-ts mutant shifted at restrictive temperature. Here, we report that the same set of genes requires a functional CCL1 gene product to be transcribed. These findings, added to previously published data, establishes that Kin28p is a cyclin-dependent kinase (CDK) with Ccl1p as a companion, both of them being necessary for general transcription and CTD phosphorylation.

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