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Direct observation of TALE protein dynamics reveals a two-state search mechanism

机译:直接观察TALE蛋白质动力学揭示了两种状态的搜索机制

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摘要

Transcription activator-like effector (TALE) proteins are a class of programmable DNA-binding proteins for which the fundamental mechanisms governing the search process are not fully understood. Here we use single-molecule techniques to directly observe TALE search dynamics along DNA templates. We find that TALE proteins are capable of rapid diffusion along DNA using a combination of sliding and hopping behaviour, which suggests that the TALE search process is governed in part by facilitated diffusion. We also observe that TALE proteins exhibit two distinct modes of action during the search process-a search state and a recognition state-facilitated by different subdomains in monomeric TALE proteins. Using TALE truncation mutants, we further demonstrate that the N-terminal region of TALEs is required for the initial non-specific binding and subsequent rapid search along DNA, whereas the central repeat domain is required for transitioning into the site-specific recognition state.
机译:转录激活因子样效应物(TALE)蛋白是一类可编程的DNA结合蛋白,其控制搜索过程的基本机制尚不完全清楚。在这里,我们使用单分子技术直接沿着DNA模板观察TALE搜索动力学。我们发现,使用滑动和跳跃行为的组合,TALE蛋白能够沿着DNA快速扩散,这表明TALE搜索过程部分受促进扩散的支配。我们还观察到,TALE蛋白在搜索过程中表现出两种不同的作用模式-搜索状态和识别状态,这些状态由单体TALE蛋白中的不同子域促进。使用TALE截短突变体,我们进一步证明TALE的N端区域是最初的非特异性结合和随后沿DNA的快速搜索所必需的,而中央重复域则是过渡到位点特异性识别状态所必需的。

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