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人类疱疹病毒DNA分子的结构组织

Structural organization of human herpesvirus DNA molecules.

作者信息

Hayward G S, Ambinder R, Ciufo D, Hayward S D, LaFemina R L

出版信息

J Invest Dermatol. 1984 Jul;83(1 Suppl):29s-41s. doi: 10.1111/1523-1747.ep12281149.

Abstract

The herpesviruses are among the largest and most complex of all DNA viruses, and their genomes display an astonishing diversity in size, structure, and organization. In 1974, the features of large inverted repeats and structural isomerization were first discovered, and these proved to be characteristic properties of many herpesvirus genomes. Since then, research using the powerful techniques of modern molecular biology has revealed a great deal of comparative structural information about the arrangement of repetitive sequences and the location, structure, and primary nucleotide sequences of the genes for several easily assayed or abundantly expressed gene products. Extensive restriction enzyme cleavage maps and complete sets of cloned DNA fragments have been constructed for each of the five human herpesviruses, HSV-1, HSV-2, CMV, EBV, and VZV, and the entire 175,000-bp nucleotide sequence of EBV DNA has been determined. Based on these maps and reagents, the procedures of "DNA fingerprinting" and "dot hybridization" are proving useful at a clinical level for characterization of isolates and studying herpesvirus epidemiology. Strain differences, localized heterogeneity, tandem-repeat-defective genomes, and sites of cell-virus DNA homology have been described in some detail. The attention of basic researchers is now turning to equating structure with function, and rapid progress is expected in studies aimed at a better understanding of the mechanisms of viral DNA replication, maintenance of the latent state, reactivation, transformation, packaging, and regulation of the lytic cycle, etc using cloned functionally active DNA fragments, isolated intact genes and promoters, and DNA transfection and in vitro expression systems.

摘要

疱疹病毒是所有DNA病毒中最大且最复杂的病毒之一,其基因组在大小、结构和组织方面展现出惊人的多样性。1974年,首次发现了大型反向重复序列和结构异构化的特征,事实证明这些是许多疱疹病毒基因组的特性。从那时起,运用现代分子生物学的强大技术开展的研究揭示了大量关于重复序列排列以及几种易于检测或大量表达的基因产物的基因位置、结构和一级核苷酸序列的比较结构信息。已为五种人类疱疹病毒,即单纯疱疹病毒1型(HSV-1)、单纯疱疹病毒2型(HSV-2)、巨细胞病毒(CMV)、EB病毒(EBV)和水痘-带状疱疹病毒(VZV)构建了广泛的限制性内切酶切割图谱和完整的克隆DNA片段集,并且已确定了EBV DNA的完整175,000碱基对核苷酸序列。基于这些图谱和试剂,“DNA指纹图谱”和“点杂交”程序在临床层面对于分离株的鉴定和疱疹病毒流行病学研究正证明是有用的。已经较为详细地描述了毒株差异、局部异质性、串联重复缺陷基因组以及细胞-病毒DNA同源性位点。基础研究人员目前正将注意力转向使结构与功能等同,并且预计在旨在更好地理解病毒DNA复制、潜伏状态维持、再激活、转化、包装以及裂解周期调控等机制的研究中,利用克隆的功能活性DNA片段、分离的完整基因和启动子以及DNA转染和体外表达系统将会取得快速进展。

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