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铁取代神经锌指因子 1 的功能特征:金属和 DNA 结合。

Functional characterization of iron-substituted neural zinc finger factor 1: metal and DNA binding.

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy, University of Maryland, Baltimore, MD 21201, USA.

出版信息

J Biol Inorg Chem. 2010 May;15(4):583-90. doi: 10.1007/s00775-010-0626-1. Epub 2010 Mar 13.

Abstract

Neural zinc finger factor 1 (NZF-1) is a nonclassical zinc finger protein involved in neuronal development. NZF-1 contains multiple copies of a unique CCHHC zinc-binding domain that recognize a promoter element in the beta-retinoic acid receptor gene termed beta-retinoic acid receptor element (beta-RARE). Previous studies have established that a two-domain fragment of NZF-1 bound with zinc is sufficient for specific DNA binding. Proper functioning of the nervous system relies heavily on iron and misregulation of this highly redox active metal has serious consequences. Several classes of zinc finger proteins have been shown to bind other metal ions, including iron. To determine if ferrous iron can coordinate to the metal-binding sites of NZF-1 and assess the functional consequences of such coordination, a fragment of NZF-1 that contains two zinc-binding domains, NZF-1 double finger (NZF-1-DF), was prepared. UV-vis spectroscopy experiments demonstrated that Fe(II) is capable of binding to NZF-1-DF. Upon reconstitution with either Fe(II) or Zn(II), NZF-1-DF binds selectively and tightly (nanomolar affinity) to its target beta-RARE DNA sequence, whereas apo-NZF-1-DF does not bind to DNA and instead aggregates.

摘要

神经锌指因子 1(NZF-1)是一种参与神经元发育的非经典锌指蛋白。NZF-1 包含多个独特的 CCHHC 锌结合域,可识别视黄酸受体基因中的启动子元件,称为视黄酸受体元件(β-RARE)。先前的研究已经证实,与锌结合的 NZF-1 的两个结构域片段足以进行特异性 DNA 结合。神经系统的正常功能在很大程度上依赖于铁,而这种高度氧化还原活性金属的失调会产生严重的后果。已经证明,几类锌指蛋白可以结合其他金属离子,包括铁。为了确定亚铁离子是否可以与 NZF-1 的金属结合位点配位,并评估这种配位的功能后果,制备了含有两个锌结合域的 NZF-1 片段 NZF-1 双指(NZF-1-DF)。紫外可见光谱实验表明,Fe(II)能够与 NZF-1-DF 结合。用 Fe(II)或 Zn(II)再构成时,NZF-1-DF 选择性且紧密地(纳摩尔亲和力)结合其靶标β-RARE DNA 序列,而无金属的 NZF-1-DF 不与 DNA 结合,而是聚集。

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