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走向工程化锌指蛋白的治疗应用。

Towards therapeutic applications of engineered zinc finger proteins.

作者信息

Klug A

机构信息

MRC Laboratory of Molecular Biology, Hills Road, Cambridge CB2 2QH, UK.

出版信息

FEBS Lett. 2005 Feb 7;579(4):892-4. doi: 10.1016/j.febslet.2004.10.104.

Abstract

It has long been the goal of molecular biologists to design DNA-binding proteins for the specific control of gene expression. The zinc finger design is ideally suited for such purposes, discriminating between closely related sequences both in vitro and in vivo. Whereas other DNA-binding proteins generally make use of the 2-fold symmetry of the double helix, zinc fingers do not and so can be linked linearly in tandem to recognize DNA sequences of different lengths, with high fidelity. This modular design offers a large number of combinatorial possibilities for the specific recognition of DNA. By fusing zinc finger peptides to repression or activation domains, genes can be selectively targeted and switched off and on. Several recent applications of such engineered zinc finger proteins (ZFPs) are described, including the activation of vascular endothelial growth factor (VEGF) in a human cell line and an animal model. Clinical trials have recently begun on using VEGF-activating ZFPs to treat human peripheral arterial disease, by stimulating vascular growth. Also in progress are pre-clinical studies using ZFPs to target the defective genes in two monogenic disorders, SCID and SCA. The aim is to replace them in each case by a correct copy from an extrachromosomal DNA donor by means of homologous recombination. Promising results are reported.

摘要

长期以来,分子生物学家的目标是设计出用于特异性控制基因表达的DNA结合蛋白。锌指设计非常适合这一目的,它在体外和体内都能区分密切相关的序列。其他DNA结合蛋白通常利用双螺旋的二重对称性,而锌指则不然,因此可以串联线性连接,以高保真度识别不同长度的DNA序列。这种模块化设计为DNA的特异性识别提供了大量的组合可能性。通过将锌指肽与抑制或激活结构域融合,可以选择性地靶向基因并将其关闭和打开。本文描述了这种工程化锌指蛋白(ZFPs)最近的一些应用,包括在人类细胞系和动物模型中激活血管内皮生长因子(VEGF)。最近已经开始了使用VEGF激活型ZFPs治疗人类外周动脉疾病的临床试验,通过刺激血管生长来实现。使用ZFPs靶向两种单基因疾病(重症联合免疫缺陷病和脊髓小脑共济失调)中的缺陷基因的临床前研究也在进行中。目的是在每种情况下通过同源重组用来自染色体外DNA供体的正确拷贝替换它们。报告了有希望的结果。

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