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Paf1复合物对于Rad6-Bre1复合物介导的组蛋白单泛素化至关重要,而Rad6-Bre1复合物为COMPASS和Dot1p介导的组蛋白甲基化发出信号。

The Paf1 complex is essential for histone monoubiquitination by the Rad6-Bre1 complex, which signals for histone methylation by COMPASS and Dot1p.

作者信息

Wood Adam, Schneider Jessica, Dover Jim, Johnston Mark, Shilatifard Ali

机构信息

Department of Biochemistry, Saint Louis University School of Medicine, St. Louis, Missouri 63104, USA.

出版信息

J Biol Chem. 2003 Sep 12;278(37):34739-42. doi: 10.1074/jbc.C300269200. Epub 2003 Jul 21.

Abstract

Monoubiquitination of histone H2B, catalyzed by Rad6-Bre1, is required for methylation of histone H3 on lysines 4 and 79, catalyzed by the Set1-containing complex COMPASS and Dot1p, respectively. The Paf1 protein complex, which associates with RNA polymerase II, is known to be required for these histone H3 methylation events. During the early elongation stage of transcription, the Paf1 complex is required for association of COMPASS with RNA polymerase II, but the role the Paf1 complex plays at the promoter has not been clear. We present evidence that the Paf1 complex is required for monoubiquitination of histone H2B at promoters. Strains deleted for several components of the Paf1 complex are defective in monoubiquitination of histone H2B, which results in the loss of methylation of lysines 4 and 79 of histone H3. We also show that Paf1 complex is required for the interaction of Rad6 and COMPASS with RNA polymerase II. Finally, we show that the Paf1 complex is required for Rad6-Bre1 catalytic activity but not for the recruitment of Rad6-Bre1 to promoters. Thus, in addition to its role during the elongation phase of transcription, the Paf1 complex appears to activate the function but not the placement of the Rad6-Bre1 ubiquitin-protein ligase at the promoters of active genes.

摘要

由Rad6-Bre1催化的组蛋白H2B单泛素化作用,分别是由含Set1的复合物COMPASS和Dot1p催化的组蛋白H3赖氨酸4和79甲基化所必需的。已知与RNA聚合酶II相关的Paf1蛋白复合物是这些组蛋白H3甲基化事件所必需的。在转录的早期延伸阶段,COMPASS与RNA聚合酶II的结合需要Paf1复合物,但Paf1复合物在启动子处发挥的作用尚不清楚。我们提供的证据表明,启动子处组蛋白H2B的单泛素化作用需要Paf1复合物。缺失Paf1复合物几个组分的菌株在组蛋白H2B单泛素化方面存在缺陷,这导致组蛋白H3赖氨酸4和79甲基化的丧失。我们还表明,Rad6和COMPASS与RNA聚合酶II的相互作用需要Paf1复合物。最后,我们表明Paf1复合物是Rad6-Bre1催化活性所必需的,但不是将Rad6-Bre1募集到启动子所必需。因此,除了其在转录延伸阶段的作用外,Paf1复合物似乎还能激活Rad6-Bre1泛素蛋白连接酶在活性基因启动子处的功能,但不是其定位。

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