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通过功能分析探究HIV-1 Rev反式激活蛋白的结构

Probing the structure of the HIV-1 Rev trans-activator protein by functional analysis.

作者信息

Thomas S L, Hauber J, Casari G

机构信息

SANDOZ Research Insitute, Department of Immunodermatology, Vienna, Austria.

出版信息

Protein Eng. 1997 Feb;10(2):103-7. doi: 10.1093/protein/10.2.103.

Abstract

Human immunodeficiency virus type 1 (HIV-1) encodes a trans-acting regulatory protein, termed Rev, which is critically required for virus replication. Rev is a sequence-specific RNA binding protein which mediates the nuclear export of unspliced and incompletely spliced viral mRNAs encoding the viral structural proteins. While CD and fluorescence measurements have provided several possible structural models of Rev, all attempts employing X-ray crystallography and NMR techniques have so far failed to provide more accurate data. We present a new approach to validate alternative structural models of the N-terminal region of Rev which contains the nuclear localization/RNA binding domain. Points of contact between structural elements in a protein were determined by introduction of targeted amino acid substitutions and subsequent scoring of the biological activities. Our data resulted in the suggestion of a new and more refined model of HIV-1 Rev structure which to date has been impossible to obtain by other means.

摘要

1型人类免疫缺陷病毒(HIV-1)编码一种反式作用调节蛋白,称为Rev,它是病毒复制所必需的关键蛋白。Rev是一种序列特异性RNA结合蛋白,介导编码病毒结构蛋白的未剪接和不完全剪接的病毒mRNA的核输出。虽然圆二色光谱(CD)和荧光测量提供了Rev的几种可能结构模型,但迄今为止,所有采用X射线晶体学和核磁共振(NMR)技术的尝试都未能提供更准确的数据。我们提出了一种新方法来验证Rev N端区域的替代结构模型,该区域包含核定位/RNA结合结构域。通过引入靶向氨基酸取代并随后对生物活性进行评分,确定了蛋白质中结构元件之间的接触点。我们的数据提示了一种新的、更精细的HIV-1 Rev结构模型,而这是迄今为止通过其他方法无法获得的。

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