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From the Cover: Design of polyzinc finger peptides with structured linkers

机译:从封面开始:具有结构化接头的多锌指肽的设计

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摘要

Zinc finger domains are perhaps the most versatile of all known DNA binding domains. By fusing up to six zinc finger modules, which normally recognize up to 18 bp of DNA, designer transcription factors can be produced to target unique sequences within large genomes. However, not all continuous DNA sequences make good zinc finger binding sites. To avoid having to target unfavorable DNA sequences, we designed multizinc finger peptides with linkers capable of spanning long stretches of nonbound DNA. Two three-finger domains were fused by using either transcription factor IIIA for the Xenopus 5S RNA gene (TFIIIA) finger 4 or a non-sequence-specific zinc finger as a “structured” linker. Our gel-shift results demonstrate that these peptides are able to bind with picomolar affinities to target sequences containing 0–10 bp of nonbound DNA. Furthermore, these peptides display greater sequence selectivity and bind with higher affinity than similar six-finger peptides containing long, flexible linkers. These peptides are likely to be of use in understanding the behavior of polydactyl proteins in nature and in the targeting of human, animal, or plant genomes for numerous applications. We also suggest that in certain polydactyl peptides an individual finger can “flip” out of the major groove to allow its neighbors to bind shorter, nontarget DNA sequences.
机译:锌指结构域可能是所有已知DNA结合结构域中功能最丰富的。通过融合最多六个锌指模块(通常可识别最多18 bp的DNA),可以产生设计者转录因子以靶向大型基因组中的独特序列。但是,并非所有连续的DNA序列都具有良好的锌指结合位点。为了避免靶向不利的DNA序列,我们设计了具有连接子的多锌指状肽,该连接子能够跨越长链未结合的DNA。通过使用非洲爪蟾5S RNA基因(TFIIIA)指4的转录因子IIIA或非序列特异性锌指作为“结构化”接头,融合两个三指结构域。我们的凝胶位移结果表明,这些肽能够以皮摩尔亲和力结合至含有0–10 bp非结合DNA的靶序列。此外,与含有长且柔性接头的类似六指肽相比,这些肽显示出更高的序列选择性并以更高的亲和力结合。这些肽可能会用于了解多指蛋白在自然界中的行为以及对人,动物或动物的靶向。 植物基因组的众多应用。我们还建议 某些手指可以“翻转”某些聚半乳糖肽 的主要凹槽,以使其邻居能够绑定较短的非目标 DNA序列。

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