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δRNA中的新型三级结构可能作为一种核酶控制元件发挥作用。

The novel tertiary structure in delta RNA may function as a ribozyme control element.

作者信息

Branch A D, Levine B J, Baroudy B M, Buckler-White A, Gerin J L, Robertson H D

机构信息

Laboratory for Studies of the Biology of Addictive Diseases, Rockefeller Univ., New York, NY.

出版信息

Prog Clin Biol Res. 1991;364:257-64.

PMID:2020701
Abstract

The viroid-like domain making up the lefthand end of the delta hepatitis genome (Branch et al., 1989) has structural elements whose interactions may be essential for replication. This portion of the genome is highly conserved in primary sequence and contains two well-defined types of structural features: sites capable of self-cleavage, and those forming a UV-sensitive element of local tertiary structure which is very stable and contains non-Watson:Crick bonds that may form a distinctive surface for binding specific proteins. The proximity of the tertiary structure to the genomic self-cleavage site suggests that the photoreactive element may regulate the ribozyme. This element's stability would limit "breathing" in this region of the circular genome, maintaining the ribozyme in the "off" conformation; its tight structure could be relieved by protein binding at the time of replication. We previously mapped a novel local tertiary structure to a highly conserved portion of the viroid genome (Branch et al., 1985). The many additional properties shared by viroids, related infectious circular RNAs of plants, and the delta agent are discussed in a recent article (Branch et al., in press-a).

摘要

构成丁型肝炎病毒基因组左手端的类病毒样结构域(Branch等人,1989年)具有一些结构元件,其相互作用可能对复制至关重要。基因组的这一部分在一级序列上高度保守,包含两种明确的结构特征类型:能够自我切割的位点,以及形成局部三级结构中对紫外线敏感的元件,该元件非常稳定,包含非沃森-克里克碱基对,可能形成用于结合特定蛋白质的独特表面。三级结构与基因组自我切割位点的接近表明,光反应元件可能调节核酶。该元件的稳定性会限制环状基因组这一区域的“呼吸”,使核酶保持在“关闭”构象;在复制时,蛋白质结合可缓解其紧密结构。我们之前将一种新的局部三级结构定位到类病毒基因组的一个高度保守部分(Branch等人,1985年)。最近的一篇文章(Branch等人,即将发表-a)讨论了类病毒、相关的植物感染性环状RNA和丁型肝炎病毒所共有的许多其他特性。

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