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利用体内和体外的缺失和嵌合体构建物分析 DEAD-box RNA“解旋酶”的功能区域。

Analyses of the functional regions of DEAD-box RNA "helicases" with deletion and chimera constructs tested in vivo and in vitro.

机构信息

Institut de Biologie Physico-chimique, CNRS UPR9073, Paris 75005, France.

出版信息

J Mol Biol. 2011 Oct 21;413(2):451-72. doi: 10.1016/j.jmb.2011.08.032. Epub 2011 Aug 23.

DOI:10.1016/j.jmb.2011.08.032
PMID:21884706
Abstract

The DEAD-box family of putative RNA helicases is composed of ubiquitous proteins that are found in nearly all organisms and that are involved in virtually all processes involving RNA. They are characterized by two tandemly linked, RecA-like domains that contain 11 conserved motifs and highly variable amino- and carboxy-terminal flanking sequences. For this reason, they are often considered to be modular multi-domain proteins. We tested this by making extensive BLASTs and sequence alignments to elucidate the minimal functional unit in nature. We then used this information to construct chimeras and deletions of six essential yeast proteins that were assayed in vivo. We purified many of the different constructs and characterized their biochemical properties in vitro. We found that sequence elements can only be switched between closely related proteins and that the carboxy-terminal sequences are important for high ATPase and strand displacement activities and for high RNA binding affinity. The amino-terminal elements were often toxic when overexpressed in vivo, and they may play regulatory roles. Both the amino and the carboxyl regions have a high frequency of sequences that are predicted to be intrinsically disordered, indicating that the flanking regions do not form distinct modular domains but probably assume an ordered structure with ligand binding. Finally, the minimal functional unit of the DEAD-box core starts two amino acids before the isolated phenylalanine of the Q motif and extends to about 35 residues beyond motif VI. These experiments provide evidence for how a highly conserved structural domain can be adapted to different cellular needs.

摘要

DEAD -box 家族的假定 RNA 解旋酶由普遍存在的蛋白质组成,几乎存在于所有生物体中,参与涉及 RNA 的几乎所有过程。它们的特征是两个串联的 RecA 样结构域,包含 11 个保守基序和高度可变的氨基末端和羧基末端侧翼序列。因此,它们通常被认为是模块化的多结构域蛋白。我们通过进行广泛的 BLAST 和序列比对来测试这一点,以阐明自然界中最小的功能单位。然后,我们使用这些信息构建了六个必需的酵母蛋白的嵌合体和缺失体,并在体内进行了检测。我们纯化了许多不同的构建体,并在体外表征了它们的生化特性。我们发现,序列元件只能在密切相关的蛋白质之间进行交换,并且羧基末端序列对于高 ATP 酶和链位移活性以及高 RNA 结合亲和力很重要。氨基末端元件在体内过表达时通常有毒,它们可能发挥调节作用。氨基和羧基区域都有很高比例的序列被预测为固有无序的,这表明侧翼区域不形成独特的模块化结构域,而是可能与配体结合形成有序结构。最后,DEAD 盒核心的最小功能单位从 Q 基序的孤立苯丙氨酸前两个氨基酸开始,延伸到大约 motif VI 之外 35 个残基。这些实验为高度保守的结构域如何适应不同的细胞需求提供了证据。

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