Updated understanding of the protein–DNA recognition code used by C2H2 zinc finger proteins

IF 6.1 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Xing Zhang , Robert M. Blumenthal , Xiaodong Cheng
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引用次数: 0

Abstract

C2H2 zinc-finger (ZF) proteins form the largest family of DNA-binding transcription factors coded by mammalian genomes. In a typical DNA-binding ZF module, there are twelve residues (numbered from −1 to −12) between the last zinc-coordinating cysteine and the first zinc-coordinating histidine. The established C2H2-ZF “recognition code” suggests that residues at positions −1, −4, and −7 recognize the 5′, central, and 3′ bases of a DNA base-pair triplet, respectively. Structural studies have highlighted that additional residues at positions −5 and −8 also play roles in specific DNA recognition. The presence of bulky and either charged or polar residues at these five positions determines specificity for given DNA bases: guanine is recognized by arginine, lysine, or histidine; adenine by asparagine or glutamine; thymine or 5-methylcytosine by glutamate; and unmodified cytosine by aspartate. This review discusses recent structural characterizations of C2H2-ZFs that add to our understanding of the principles underlying the C2H2-ZF recognition code.

Abstract Image

对 C2H2 锌指蛋白使用的蛋白质-DNA 识别代码的最新了解
C2H2 锌指(ZF)蛋白是哺乳动物基因组中最大的 DNA 结合转录因子家族。在一个典型的 DNA 结合 ZF 模块中,最后一个锌配位半胱氨酸和第一个锌配位组氨酸之间有 12 个残基(编号从 -1 到 -12)。根据已确立的 C2H2-ZF "识别码",位于-1、-4 和-7 位置的残基分别能识别 DNA 碱基对三元组中的 5′、中心和 3′碱基。结构研究表明,位于 -5 和 -8 位的其他残基也在特异性 DNA 识别中发挥作用。精氨酸、赖氨酸或组氨酸可识别鸟嘌呤;天冬酰胺或谷氨酰胺可识别腺嘌呤;谷氨酸可识别胸腺嘧啶或 5-甲基胞嘧啶;天冬氨酸可识别未修饰的胞嘧啶。本综述讨论了 C2H2-ZFs 的最新结构特征,这些特征加深了我们对 C2H2-ZF 识别代码基本原理的理解。
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来源期刊
Current opinion in structural biology
Current opinion in structural biology 生物-生化与分子生物学
CiteScore
12.20
自引率
2.90%
发文量
179
审稿时长
6-12 weeks
期刊介绍: Current Opinion in Structural Biology (COSB) aims to stimulate scientifically grounded, interdisciplinary, multi-scale debate and exchange of ideas. It contains polished, concise and timely reviews and opinions, with particular emphasis on those articles published in the past two years. In addition to describing recent trends, the authors are encouraged to give their subjective opinion of the topics discussed. In COSB, we help the reader by providing in a systematic manner: 1. The views of experts on current advances in their field in a clear and readable form. 2. Evaluations of the most interesting papers, annotated by experts, from the great wealth of original publications. [...] The subject of Structural Biology is divided into twelve themed sections, each of which is reviewed once a year. Each issue contains two sections, and the amount of space devoted to each section is related to its importance. -Folding and Binding- Nucleic acids and their protein complexes- Macromolecular Machines- Theory and Simulation- Sequences and Topology- New constructs and expression of proteins- Membranes- Engineering and Design- Carbohydrate-protein interactions and glycosylation- Biophysical and molecular biological methods- Multi-protein assemblies in signalling- Catalysis and Regulation
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