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首页> 外文期刊>Virology >MuLV IN mutants responsive to HDAC inhibitors enhance transcription from unintegrated retroviral DNA
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MuLV IN mutants responsive to HDAC inhibitors enhance transcription from unintegrated retroviral DNA

机译:对HDAC抑制剂有反应的MuLV IN突变体可增强未整合的逆转录病毒DNA的转录

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For Moloney murine leukemia virus (M-MuLV), sustained viral infections require expression from an integrated provirus. For many applications, non-integrating retroviral vectors have been utilized to avoid the unwanted effects of integration, however, the level of expression from unintegrated DNA is significantly less than that of integrated provirus. We find that unintegrated DNA expression can be increased in the presence of HDAC inhibitors, such as TSA, when applied in combination with integrase (IN) mutations. These mutants include an active site mutation as well as catalytically active INs bearing mutations of K376 in the MuLV C-terminal domain of IN. MuLV IN K376 is homologous to K266 in HIV-1 IN, a known substrate for acetylation. The MuLV IN protein is acetylated by p300 in vitro, however, the effect of HDAC inhibitors on gene expression from unintegrated DNA is not dependent on the acetylation state of MuLV IN K376.
机译:对于莫洛尼氏鼠白血病病毒(M-MuLV),持续的病毒感染需要从整合的原病毒中表达。对于许多应用,已经利用非整合的逆转录病毒载体来避免整合的有害作用,但是,来自非整合DNA的表达水平显着低于整合前病毒的表达水平。我们发现,当与整合酶(IN)突变结合应用时,在HDAC抑制剂(例如TSA)存在下可以增加未整合的DNA表达。这些突变体包括一个活性位点突变以及在IN的MuLV C末端结构域中带有K376突变的催化活性IN。 MuLV IN K376与HIV-1 IN(已知的乙酰化底物)中的K266同源。 MuLV IN蛋白在体外被p300乙酰化,但是,HDAC抑制剂对未整合DNA的基因表达的影响并不取决于MuLV IN K376的乙酰化状态。

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