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首页> 外文期刊>Cold Spring Harbor symposia on quantitative biology. >A Transcription Fork Model for Pol IV and Pol V-Dependent RNA-Directed DNA Methylation
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A Transcription Fork Model for Pol IV and Pol V-Dependent RNA-Directed DNA Methylation

机译:Pol IV和Pol V依赖的RNA定向DNA甲基化的转录叉模型

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In Arabidopsis thaliana, nuclear multisubunit RNA polymerase IV (Pol IV) and RNA-DEPENDENT RNA POLYMERASE 2 (RDR2) are required for the biogenesis of 24-nucleotide small interfering RNAs (siRNAs) that direct DNA methylation and transcriptional silencing at target loci transcribed by nuclear multisubunit RNA polymerase V (Pol V). Pol IV and RDR2 physically associate and RDR2's polymerase activity in vitro is dependent on Pol IV. RDR2 transcription of nascent Pol IV transcripts might result in discontinuous second strands, analogous to lagging-strand Okazaki fragments generated during DNA replication. In vitro, Pol V is unable to displace nontemplate DNA during transcriptional elongation. This suggests a need for DNA duplex unwinding by helper proteins, perhaps analogous to the helicase-mediated duplex unwinding that occurs at replication forks to enable leading strand synthesis by DNA polymerase e. A multiprotein complex (DRD1, DMS3, DMS11, RDM1) known to enable Pol V transcription might facilitate duplex unwinding via ATP-dependent DNA translocase, single-stranded DNA binding, and cohesin-like strand capture activities. These considerations are discussed and incorporated into a "transcription fork" model for Pol IV and Pol V-dependent RNA-directed DNA methylation.
机译:在拟南芥中,需要核多亚基RNA聚合酶IV(Pol IV)和依赖RNA的RNA聚合酶2(RDR2)来实现24核苷酸小干扰RNA(siRNA)的生物合成,该小干扰RNA指导DNA甲基化和转录沉默,该靶点由核多亚基RNA聚合酶V(Pol V)。 Pol IV和RDR2在物理上缔合,并且体外RDR2的聚合酶活性取决于Pol IV。新生Pol IV转录本的RDR2转录可能导致不连续的第二条链,类似于DNA复制过程中产生的落后链Okazaki片段。在体外,Pol V无法在转录延伸过程中置换非模板DNA。这表明需要通过辅助蛋白解链DNA双链,可能类似于在复制叉处发生的解旋酶介导的双链解链,以使DNA聚合酶能够进行前导链合成。已知能够实现Pol V转录的多蛋白复合物(DRD1,DMS3,DMS11,RDM1)可能通过ATP依赖的DNA转移酶,单链DNA结合和粘着蛋白样链捕获活性促进双链解绕。讨论了这些考虑因素,并将这些考虑因素纳入了针对Pol IV和Pol V依赖的RNA指导的DNA甲基化的“转录叉”模型。

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