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Organization of the human mitochondrial transcription initiation complex

机译:人线粒体转录起始复合物的组织

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Initiation of transcription in human mitochondria involves two factors, TFAM and TFB2M, in addition to the mitochondrial RNA polymerase, POLRMT. We have investigated the organization of the human mitochondrial transcription initiation complex on the light-strand promoter (LSP) through solution X-ray scattering, electron microscopy (EM) and biochemical studies. Our EM results demonstrate a compact organization of the initiation complex, suggesting that protein-protein interactions might help mediate initiation. We demonstrate that, in the absence of DNA, only POLRMT and TFAM form a stable interaction, albeit one with low affinity. This is consistent with the expected transient nature of the interactions necessary for initiation and implies that the promoter DNA acts as a scaffold that enables formation of the full initiation complex. Docking of known crystal structures into our EM maps results in a model for transcriptional initiation that strongly correlates with new and existing biochemical observations. Our results reveal the organization of TFAM, POLRMT and TFB2M around the LSP and represent the first structural characterization of the entire mitochondrial transcriptional initiation complex.
机译:除了线粒体RNA聚合酶POLRMT之外,人线粒体中转录的启动还涉及两个因素,TFAM和TFB2M。我们已经通过溶液X射线散射,电子显微镜(EM)和生化研究研究了在光链启动子(LSP)上人类线粒体转录起始复合物的组织。我们的电磁结果证明了起始复合物的紧密组织,表明蛋白质-蛋白质相互作用可能有助于介导起始。我们证明,在不存在DNA的情况下,只有POLRMT和TFAM可以形成稳定的相互作用,尽管亲和力较低。这与引发必需的相互作用的预期的瞬时性质是一致的,并且暗示启动子DNA充当能够形成完整的引发复合物的支架。将已知的晶体结构对接到我们的EM谱图中,就形成了一个转录起始模型,该模型与新的和现有的生化观察密切相关。我们的结果揭示了围绕LSP的TFAM,POLRMT和TFB2M的组织,并代表了整个线粒体转录起始复合物的第一个结构特征。

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