丁型肝炎病毒基因组RNA的细胞内切割与连接:顺式作用序列和宿主因子对核酶活性的调控
Intracellular cleavage and ligation of hepatitis delta virus genomic RNA: regulation of ribozyme activity by cis-acting sequences and host factors.
作者信息
Lazinski D W, Taylor J M
机构信息
Fox Chase Cancer Center, Philadelphia, Pennsylvania 19111-2497.
出版信息
J Virol. 1995 Feb;69(2):1190-200. doi: 10.1128/JVI.69.2.1190-1200.1995.
Abstract
During replication, a ribozyme within the genomic RNA of hepatitis delta virus cleaves multimeric precursors to release a unit-length linear intermediate. Intramolecular ligation of this intermediate produces the circular genomic RNA. Although one copy of the ribozyme is reconstituted by such ligation, it does not subsequently cleave and destroy the circular conformation. We have identified cis-acting attenuator sequences that prevent self-cleavage of the circular product by base pairing with and inactivating the ribozyme. Furthermore, we have shown that during the initial processing of the multimeric precursor RNA, host-specific factors activate the ribozyme by preventing its association with the attenuator sequences. Thus, we demonstrate a novel switching mechanism that regulates ribozyme activity inside the cell.
摘要
在复制过程中,丁型肝炎病毒基因组RNA中的一种核酶切割多聚体前体以释放单位长度的线性中间体。该中间体的分子内连接产生环状基因组RNA。虽然通过这种连接可重构一份核酶,但它随后不会切割并破坏环状构象。我们已经鉴定出顺式作用衰减子序列,其通过与核酶碱基配对并使其失活来阻止环状产物的自我切割。此外,我们已经表明,在多聚体前体RNA的初始加工过程中,宿主特异性因子通过阻止其与衰减子序列结合来激活核酶。因此,我们证明了一种调节细胞内核酶活性的新型开关机制。
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Intracellular cleavage and ligation of hepatitis delta virus genomic RNA: regulation of ribozyme activity by cis-acting sequences and host factors.丁型肝炎病毒基因组RNA的细胞内切割与连接:顺式作用序列和宿主因子对核酶活性的调控
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