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从抑制结构域到定制锌指蛋白:一种针对HIV的细胞内免疫新策略。

From repression domains to designer zinc finger proteins: a novel strategy of intracellular immunization against HIV.

作者信息

Thiesen H J

机构信息

Institut für Immunologie, Rostock, Germany.

出版信息

Gene Expr. 1996;5(4-5):229-43.

PMID:8723389
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6138030/
Abstract

Tissue-specific gene regulation of eukaryotic organisms is to a large extent mediated by transcription factors that interact with genomic DNA sequences in a sequence-specific manner. The purpose of this synopsis is to put forward the potential of designer zinc finger proteins in treating infections of human immunodeficiency virus (HIV). Artificial transcription factors containing designer zinc finger structures fused to activator or repressor domains have been designated Transcription Response Modifiers (TRMs). The principle of engineering TRMs has been derived from the analysis of human Krüppel-type zinc finger genes and their products. Our research efforts encompass two fascinating features that are displayed by the human Krüppel-type zinc finger protein KOX1: 1) the Krüppel-type zinc finger domains display rules of sequence-specific DNA recognition, and 2) the evolutionarily conserved Krüppel-associated box (KRAB) presents one of the strongest transcriptional repressors identified so far in mammalian organisms. The KRAB repressor activity is postulated to be mediated through co-repressor molecules, such as Silencing Mediating Protein-1 (SMP-1). Thus, the structural organization and functional analysis of zinc finger proteins revealed principles of zinc finger transcription factors that are applicable for reducing the viral load in individuals infected with HIV. In this article, a novel concept of generating therapeutic proteins is outlined that might be conceptually promising in modulating gene expressions of any kind.

摘要

真核生物的组织特异性基因调控在很大程度上是由转录因子介导的,这些转录因子以序列特异性的方式与基因组DNA序列相互作用。本综述的目的是提出设计锌指蛋白在治疗人类免疫缺陷病毒(HIV)感染方面的潜力。含有与激活域或抑制域融合的设计锌指结构的人工转录因子被称为转录反应修饰因子(TRM)。TRM的工程原理源自对人类Krüppel型锌指基因及其产物的分析。我们的研究工作围绕人类Krüppel型锌指蛋白KOX1所展现的两个引人入胜的特征展开:1)Krüppel型锌指结构域呈现序列特异性DNA识别规则;2)进化上保守的Krüppel相关框(KRAB)是迄今为止在哺乳动物中鉴定出的最强转录抑制因子之一。据推测,KRAB的抑制活性是通过共抑制分子介导的,如沉默介导蛋白-1(SMP-1)。因此,锌指蛋白的结构组织和功能分析揭示了锌指转录因子的原理,这些原理适用于降低HIV感染个体的病毒载量。在本文中,概述了一种产生治疗性蛋白的新概念,这在调控任何类型的基因表达方面可能在概念上具有前景。

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Nat Biotechnol. 2001 Jul;19(7):656-60. doi: 10.1038/90264.

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Krab domains analyzed in human Cys/His-type zinc-finger proteins KOX 1, KOX 8, and KOX 19.在人类半胱氨酸/组氨酸型锌指蛋白KOX 1、KOX 8和KOX 19中分析的Krab结构域。
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