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Artificial zinc finger peptides: creation, DNA recognition, and gene regulation [Review]

机译:人工锌指肽:创造,DNA识别和基因调控[综述]

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Proteins control most biological reactions and the disorder of their expression level causes many diseases. The advent of genomic sequencing and the availability of the complete sequences of several genomes provide new opportunities to study biology and to develop therapeutic strategies through specific modulation of the transcription of target genes. Therefore, regulation of the transcription level by "artificial repressors" is of special importance. Of the DNA-binding motifs that have been manipulated by design or selection, Cys(2)-His(2) zinc finger proteins have demonstrated the greatest potential for manipulation into general and specific transcription factors. Of special interest is the feature that this family of proteins has modular structures and can recognize a diverse set of DNA sequences in a sequence-specific manner. Therefore, zinc finger motifs offer an attractive framework for the design of novel DNA binding proteins, and such a DNA binding protein would be expected to possess a unique binding sequence with high specificity and affinity. Principally, two approaches have been taken to the design of artificial zinc finger proteins. One is a selection strategy via phage display methods to alter the recognition sequence, and another is a structure-based linking strategy to extend the length of a DNA recognition sequence. Such novel zinc finger peptides (or proteins) offer great promise for genome-specific transcription switches in the near future. (C) 2000 Elsevier Science B.V. All rights reserved. [References: 20]
机译:蛋白质控制着大多数生物反应,其表达水平的紊乱导致许多疾病。基因组测序的出现和几个基因组完整序列的可用性为研究生物学和通过特异性调节靶基因转录提供治疗策略提供了新的机会。因此,通过“人工阻遏物”调节转录水平是特别重要的。在已经通过设计或选择操作的DNA结合基序中,Cys(2)-His(2)锌指蛋白已显示出对一般和特定转录因子进行操作的最大潜力。特别令人感兴趣的是该蛋白质家族具有模块化结构并可以以序列特异性方式识别各种DNA序列的特征。因此,锌指基序为新颖的DNA结合蛋白的设计提供了有吸引力的框架,并且期望这种DNA结合蛋白具有具有高特异性和亲和力的独特结合序列。原则上,已经采用了两种方法来设计人工锌指蛋白。一种是通过噬菌体展示方法改变识别序列的选择策略,另一种是基于结构的连接策略以延长DNA识别序列的长度。这种新颖的锌指肽(或蛋白质)在不久的将来为基因组特异性转录开关提供了广阔的前景。 (C)2000 Elsevier Science B.V.保留所有权利。 [参考:20]

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