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Ty3整合酶非保守结构域中的突变会影响Ty3生命周期的多个阶段。

Mutations in nonconserved domains of Ty3 integrase affect multiple stages of the Ty3 life cycle.

作者信息

Nymark-McMahon M H, Sandmeyer S B

机构信息

Department of Biological Chemistry, University of California, Irvine, Irvine, California 92697, USA.

出版信息

J Virol. 1999 Jan;73(1):453-65. doi: 10.1128/JVI.73.1.453-465.1999.

Abstract

Ty3, a retroviruslike element of Saccharomyces cerevisiae, transposes into positions immediately upstream of RNA polymerase III-transcribed genes. The Ty3 integrase (IN) protein is required for integration of the replicated, extrachromosomal Ty3 DNA. In retroviral IN, a conserved core region is sufficient for strand transfer activity. In this study, charged-to-alanine scanning mutagenesis was used to investigate the roles of the nonconserved amino- and carboxyl-terminal regions of Ty3 IN. Each of the 20 IN mutants was defective for transposition, but no mutant was grossly defective for capsid maturation. All mutations affecting steady-state levels of mature IN protein resulted in reduced levels of replicated DNA, even when polymerase activity was not grossly defective as measured by exogenous reverse transcriptase activity assay. Thus, IN could contribute to nonpolymerase functions required for DNA production in vivo or to the stability of the DNA product. Several mutations in the carboxyl-terminal domain resulted in relatively low levels of processed 3' ends of the replicated DNA, suggesting that this domain may be important for binding of IN to the long terminal repeat. Another class of mutants produced wild-type amounts of DNA with correctly processed 3' ends. This class could include mutants affected in nuclear entry and target association. Collectively, these mutations demonstrate that in vivo, within the preintegration complex, IN performs a central role in coordinating multiple late stages of the retrotransposition life cycle.

摘要

Ty3是酿酒酵母中的一种逆转录病毒样元件,它转座到RNA聚合酶III转录基因上游紧邻的位置。Ty3整合酶(IN)蛋白是复制后的染色体外Ty3 DNA整合所必需的。在逆转录病毒IN中,一个保守的核心区域足以进行链转移活性。在本研究中,采用电荷到丙氨酸扫描诱变来研究Ty3 IN非保守的氨基末端和羧基末端区域的作用。20个IN突变体中的每一个在转座方面都有缺陷,但没有一个突变体在衣壳成熟方面有严重缺陷。所有影响成熟IN蛋白稳态水平的突变都导致复制DNA水平降低,即使通过外源逆转录酶活性测定法测量,聚合酶活性没有严重缺陷。因此,IN可能有助于体内DNA产生所需的非聚合酶功能或DNA产物的稳定性。羧基末端结构域中的几个突变导致复制DNA的加工3'末端水平相对较低,这表明该结构域可能对IN与长末端重复序列的结合很重要。另一类突变体产生野生型数量的具有正确加工3'末端的DNA。这类突变体可能包括在核进入和靶标关联方面受影响的突变体。总的来说,这些突变表明在体内,在整合前复合物中,IN在协调逆转录转座生命周期的多个后期阶段中发挥核心作用。

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