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酿酒酵母中Rkr1的鉴定,一种与染色质修饰存在功能联系的核RING结构域蛋白。

Identification of Rkr1, a nuclear RING domain protein with functional connections to chromatin modification in Saccharomyces cerevisiae.

作者信息

Braun Mary A, Costa Patrick J, Crisucci Elia M, Arndt Karen M

机构信息

Department of Biological Sciences, University of Pittsburgh, 269 Crawford Hall, 4249 Fifth Avenue, Pittsburgh, PA 15260, USA.

出版信息

Mol Cell Biol. 2007 Apr;27(8):2800-11. doi: 10.1128/MCB.01947-06. Epub 2007 Feb 5.

Abstract

Proper transcription by RNA polymerase II is dependent on the modification state of the chromatin template. The Paf1 complex is associated with RNA polymerase II during transcription elongation and is required for several histone modifications that mark active genes. To uncover additional factors that regulate chromatin or transcription, we performed a genetic screen for mutations that cause lethality in the absence of the Paf1 complex component Rtf1. Our results have led to the discovery of a previously unstudied gene, RKR1. Strains lacking RKR1 exhibit phenotypes associated with defects in transcription and chromatin function. These phenotypes include inositol auxotrophy, impaired telomeric silencing, and synthetic lethality with mutations in SPT10, a gene that encodes a putative histone acetyltransferase. In addition, deletion of RKR1 causes severe genetic interactions with mutations that prevent histone H2B lysine 123 ubiquitylation or histone H3 lysine 4 methylation. RKR1 encodes a conserved nuclear protein with a functionally important RING domain at its carboxy terminus. In vitro experiments indicate that Rkr1 possesses ubiquitin-protein ligase activity. Taken together, our results identify a new participant in a protein ubiquitylation pathway within the nucleus that acts to modulate chromatin function and transcription.

摘要

RNA聚合酶II的正确转录取决于染色质模板的修饰状态。Paf1复合物在转录延伸过程中与RNA聚合酶II相关联,并且是几种标记活跃基因的组蛋白修饰所必需的。为了发现调控染色质或转录的其他因子,我们针对在缺乏Paf1复合物组分Rtf1时导致致死性的突变进行了遗传筛选。我们的结果导致发现了一个先前未被研究的基因RKR1。缺乏RKR1的菌株表现出与转录和染色质功能缺陷相关的表型。这些表型包括肌醇营养缺陷、端粒沉默受损以及与编码假定组蛋白乙酰转移酶的基因SPT10中的突变产生合成致死性。此外,RKR1的缺失会导致与阻止组蛋白H2B赖氨酸123泛素化或组蛋白H3赖氨酸4甲基化的突变发生严重的遗传相互作用。RKR1编码一种保守的核蛋白,在其羧基末端具有功能重要的RING结构域。体外实验表明Rkr1具有泛素-蛋白连接酶活性。综上所述,我们的结果确定了细胞核内一种蛋白质泛素化途径中的新参与者,该参与者作用于调节染色质功能和转录。

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