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Overcoming conservation in TALE–DNA interactions: a minimal repeat scaffold enables selective recognition of an oxidized 5-methylcytosine

机译:克服TALE-DNA相互作用中的保守性:最小的重复支架可以选择性识别氧化的5-甲基胞嘧啶

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摘要

Transcription-activator-like effectors (TALEs) are repeat-based proteins featuring programmable DNA binding. The repulsion of TALE repeats by 5-methylcytosine (5mC) and its oxidized forms makes TALEs potential probes for their programmable analysis. However, this potential has been limited by the inability to engineer repeats capable of actual, fully selective binding of an (oxidized) 5mC: the extremely conserved and simple nucleobase recognition mode of TALE repeats and their extensive involvement in inter-repeat interactions that stabilize the TALE fold represent major engineering hurdles. We evaluated libraries of alternative, strongly truncated repeat scaffolds and discovered a repeat that selectively recognizes 5-carboxylcytosine (5caC), enabling construction of the first programmable receptors for an oxidized 5mC. In computational studies, this unusual scaffold executes a dual function via a critical arginine that provides inter-repeat stabilization and selectively interacts with the 5caC carboxyl group via a salt-bridge. These findings argue for an unexpected adaptability of TALE repeats and provide a new impulse for the design of programmable probes for nucleobases beyond A, G, T and C.
机译:转录激活因子样效应物(TALE)是基于重复序列的蛋白质,具有可编程的DNA结合。 5-甲基胞嘧啶(5mC)排斥TALE重复序列,其氧化形式使TALE成为进行可编程分析的潜在探针。但是,这种潜力受到无法设计能够实际,完全选择性结合(氧化的)5mC的重复序列的限制:TALE重复序列极其保守且简单的核碱基识别模式,并且它们广泛参与重复序列间的相互作用,从而稳定了该序列。 TALE折痕代表了主要的工程障碍。我们评估了备选的,被强截短的重复支架的文库,发现了一个选择性识别5-羧基胞嘧啶(5caC)的重复序列,从而能够构建第一个可程序化的5mC受体。在计算研究中,这种不寻常的支架通过关键的精氨酸执行双重功能,该精氨酸提供重复序列间的稳定作用并通过盐桥选择性地与5caC羧基相互作用。这些发现证明了TALE重复序列具有出乎意料的适应性,并为设计A,G,T和C以外的核碱基的探针提供了新的动力。

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