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首页> 外文期刊>Journal of Molecular Biology >The in vitro Biochemical Characterization of an HIV-1 Restriction Factor APOBEC3F: Importance of Loop 7 on Both CD1 and CD2 for DNA Binding and Deamination
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The in vitro Biochemical Characterization of an HIV-1 Restriction Factor APOBEC3F: Importance of Loop 7 on Both CD1 and CD2 for DNA Binding and Deamination

机译:HIV-1限制因子Apobec3F的体外生化表征:DNA结合和脱胺的CD1和CD2上的环7的重要性

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APOBEC3F (A3F) is a member of the apolipoprotein B mRNA-editing enzyme catalytic polypeptide-like (APOBEC) family of proteins that can deaminate cytosine (C) to uracil (U) on nucleic acids. A3F is one of the four APOBEC members with two Zn-coordinated homologous cytosine deaminase (CD) domains, with the others being A3G, A3D, and A3B. Here we report the in vitro characterization of DNA binding and deaminase activities using purified wild-type and various mutant proteins of A3F from an Escherichia coli expression system. We show that even though CD1 is catalytically inactive and CD2 is the active deaminase domain, presence of CD1 on the N-terminus of CD2 enhances the deaminase activity by over an order of magnitude. This enhancement of CD2 catalytic activity is mainly through the increase of substrate single-stranded (ss) DNA binding by the N-terminal CD1 domain. We further show that the loop 7 of both CD1 and CD2 of A3F plays an important role for ssDNA binding for each individual domain, as well as for the deaminase activity of CD2 domain in the full-length A3F. (C) 2016 Published by Elsevier Ltd.
机译:apobec3f(a3f)是载脂蛋白b mRNA编辑酶催化多肽样(apobec)的蛋白质的成员,其可以将胞嘧啶(c)脱核(c)脱核酸核酸(u)。 A3F是具有两个Zn协调的同源胞嘧啶脱氨酶(CD)结构域的四个apobec构件之一,其它是A3G,A3D和A3B。在这里,我们通过从大肠杆菌表达系统中纯化的野生型和A3F的各种突变蛋白报告DNA结合和脱氨酶活性的体外表征。我们表明,尽管CD1是催化惰性的,CD2是活性脱氨酶结构域,CD2的N-末端对CD1的存在使脱氨酶活性超过一个数量级。这种CD2催化活性的增强主要是通过N-末端CD1结构域的底物单链(SS)DNA的增加。我们进一步表明,A3F的CD1和CD2的回路7对每个单独结构域的SSDNA结合起着重要作用,以及全长A3F中CD2结构域的脱氨酶活性。 (c)2016年由elestvier有限公司发布

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