Gu Liping, Husain-Ponnampalam Rhonda, Hoffmann-Benning Susanne, Henry R William
Department of Biochemistry & Molecular Biology, Michigan State University, East Lansing, Michigan 48824, USA.
J Biol Chem. 2007 Sep 21;282(38):27887-96. doi: 10.1074/jbc.M702269200. Epub 2007 Aug 1.
Human U6 small nuclear RNA gene transcription by RNA polymerase III requires the general transcription factor SNAP(C), which binds to human small nuclear RNA core promoter elements and nucleates pre-initiation complex assembly with the Brf2-TFIIIB complex. Multiple components in this pathway are phosphorylated by the protein kinase CK2, including the Bdp1 subunit of the Brf2-TFIIIB complex, and RNA polymerase III, with negative and positive outcomes for U6 transcription, respectively. However, a role for CK2 phosphorylation of SNAP(C) in U6 transcription has not been defined. In this report, we investigated the role of CK2 in modulating the transcriptional properties of SNAP(C) and demonstrate that within SNAP(C), CK2 phosphorylates the N-terminal half of the SNAP190 subunit at two regions (amino acids 20-63 and 514-545) that each contain multiple CK2 consensus sites. SNAP190 phosphorylation by CK2 inhibits both SNAP(C) DNA binding and U6 transcription activity. Mutational analyses of SNAP190 support a model wherein CK2 phosphorylation triggers an allosteric inhibition of the SNAP190 Myb DNA binding domain.
RNA聚合酶III对人U6小核RNA基因的转录需要通用转录因子SNAP(C),它与人小核RNA核心启动子元件结合,并与Brf2-TFIIIB复合物一起启动预起始复合物的组装。该途径中的多个组分被蛋白激酶CK2磷酸化,包括Brf2-TFIIIB复合物的Bdp1亚基和RNA聚合酶III,这对U6转录分别产生负面和正面影响。然而,CK2对SNAP(C)的磷酸化在U6转录中的作用尚未明确。在本报告中,我们研究了CK2在调节SNAP(C)转录特性中的作用,并证明在SNAP(C)中,CK2在SNAP190亚基的N端一半的两个区域(氨基酸20-63和514-545)进行磷酸化,每个区域都包含多个CK2共有位点。CK2对SNAP190的磷酸化抑制了SNAP(C)的DNA结合和U6转录活性。对SNAP190的突变分析支持了一种模型,即CK2磷酸化触发了SNAP190 Myb DNA结合结构域的变构抑制。
