Evaluation of novel design strategies for developing zinc finger nucleases tools for treating human diseases.

Biotechnology Research International Pub Date : 2014-01-01 Epub Date: 2014-04-06 DOI:10.1155/2014/970595
Christian Bach, William Sherman, Jani Pallis, Prabir Patra, Hassan Bajwa
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Abstract

Zinc finger nucleases (ZFNs) are associated with cell death and apoptosis by binding at countless undesired locations. This cytotoxicity is associated with the binding ability of engineered zinc finger domains to bind dissimilar DNA sequences with high affinity. In general, binding preferences of transcription factors are associated with significant degenerated diversity and complexity which convolutes the design and engineering of precise DNA binding domains. Evolutionary success of natural zinc finger proteins, however, evinces that nature created specific evolutionary traits and strategies, such as modularity and rank-specific recognition to cope with binding complexity that are critical for creating clinical viable tools to precisely modify the human genome. Our findings indicate preservation of general modularity and significant alteration of the rank-specific binding preferences of the three-finger binding domain of transcription factor SP1 when exchanging amino acids in the 2nd finger.

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评估用于开发治疗人类疾病的锌指核酸酶工具的新型设计策略。
锌指核酸酶(ZFNs)与无数不希望出现的位置结合,从而导致细胞死亡和凋亡。这种细胞毒性与锌指结构域的结合能力有关,它能以高亲和力结合不同的 DNA 序列。一般来说,转录因子的结合偏好与显著的退化多样性和复杂性有关,这使得精确 DNA 结合结构域的设计和工程变得复杂。然而,天然锌指蛋白的成功进化证明,大自然创造了特定的进化特征和策略,如模块化和等级特异性识别,以应对结合的复杂性。我们的研究结果表明,当交换第二指的氨基酸时,转录因子 SP1 三指结合结构域的一般模块性得以保留,而等级特异性结合偏好发生了显著变化。
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