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首页> 外文期刊>Virology >Role of mutations identified in ORFs M56 (terminase), M70 (primase) and M98 (endonuclease) in the temperature-sensitive phenotype of murine cytomegalovirus mutant tsm5.
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Role of mutations identified in ORFs M56 (terminase), M70 (primase) and M98 (endonuclease) in the temperature-sensitive phenotype of murine cytomegalovirus mutant tsm5.

机译:在ORF M56(末端酶),M70(引发酶)和M98(核酸内切酶)中鉴定出的突变在小鼠巨细胞病毒突变株tsm5的温度敏感表型中的作用。

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Twenty-six non-synonymous and synonymous mutations have been identified in the temperature-sensitive (ts) mutant (tsm5) of the K181 (Birmingham) variant of murine cytomegalovirus that is deficient in DNA synthesis, processing and packaging at the non-permissive temperature and produces undetectable levels of infectious virus in mice. Non-synonymous mutations identified in the M70 (primase), M56 (terminase) and M98 (nuclease) ORFs were introduced individually and in combination into the K181 (Perth) variant using BAC technology to examine their role in the ts phenotype. The M56 (G439R) and M98 (P324S) mutations had no evident role in the ts phenotype. However, the C890Y M70 mutation alone and in combination with the M56 and/or M98 mutations rendered the virus ts, unable to replicate in mice and highly defective in DNA synthesis. Reversion of the tyrosine mutation to cysteine or introduction of C890M (experimentally) or C890S (naturally) restored the wt phenotype.
机译:在鼠巨细胞病毒K181(伯明翰)变体的温度敏感(ts)突变体(tsm5)中鉴定出26个非同义和同义突变,该突变在非容许温度下DNA合成,加工和包装不足并在小鼠中产生检测不到水平的传染性病毒。使用BAC技术将M70(引物酶),M56(末端酶)和M98(核酸酶)ORF中识别出的非同义突变单独引入并结合到K181(珀斯)变体中,以检查它们在ts表型中的作用。 M56(G439R)和M98(P324S)突变在ts表型中没有明显作用。但是,单独的C890Y M70突变以及与M56和/或M98突变的结合会导致ts病毒,无法在小鼠中复制并且在DNA合成中高度缺陷。将酪氨酸突变回复为半胱氨酸或引入C890M(实验性地)或C890S(自然地)恢复了wt表型。

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