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A novel intermediate in transcription initiation by human mitochondrial RNA polymerase

机译:人线粒体RNA聚合酶转录起始的新型中间体

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摘要

The mitochondrial genome is transcribed by a single-subunit T7 phage-like RNA polymerase (mtRNAP), structurally unrelated to cellular RNAPs. In higher eukaryotes, mtRNAP requires two transcription factors for efficient initiation—TFAM, a major nucleoid protein, and TFB2M, a transient component of mtRNAP catalytic site. The mechanisms behind assembly of the mitochondrial transcription machinery and its regulation are poorly understood. We isolated and identified a previously unknown human mitochondrial transcription intermediate—a pre-initiation complex that includes mtRNAP, TFAM and promoter DNA. Using protein–protein cross-linking, we demonstrate that human TFAM binds to the N-terminal domain of mtRNAP, which results in bending of the promoter DNA around mtRNAP. The subsequent recruitment of TFB2M induces promoter melting and formation of an open initiation complex. Our data indicate that the pre-initiation complex is likely to be an important target for transcription regulation and provide basis for further structural, biochemical and biophysical studies of mitochondrial transcription.
机译:线粒体基因组由单亚基T7噬菌体样RNA聚合酶(mtRNAP)转录,该结构与细胞RNAP无关。在高等真核生物中,mtRNAP需要两个转录因子才能有效启动,即主要的类核蛋白TFAM和mtRNAP催化位点的瞬时成分TFB2M。线粒体转录机制组装及其调控背后的机制了解甚少。我们分离并鉴定了一个以前未知的人类线粒体转录中间体,这是一种包括mtRNAP,TFAM和启动子DNA的预启动复合物。使用蛋白质-蛋白质交联,我们证明了人TFAM与mtRNAP的N末端结构域结合,这导致mtRNAP周围的启动子DNA弯曲。随后募集的TFB2M诱导启动子融化并形成开放起始复合物。我们的数据表明,起始前复合物可能是转录调控的重要目标,并为线粒体转录的进一步结构,生化和生物物理研究提供基础。

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