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Mouse Cytomegalovirus Crosses the Species Barrier with Help from a Few Human Cytomegalovirus Proteins

机译:小鼠巨细胞病毒在少数人类巨细胞病毒蛋白的帮助下越过了物种壁垒

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摘要

Strong species specificity and similar tropisms suggest mouse cytomegalovirus (mCMV) as a potential vector for transgenes into human cells. We reexamined the dogma that mouse cytomegalovirus cannot productively replicate in human cells and found that mouse cytomegalovirus can produce infectious particles albeit at a level that does not sustain an infection. This finding demonstrates that mouse cytomegalovirus can undergo all processes of its life cycle in human cells but may not be well adapted to circumvent the human cell's intrinsic defenses. The suppression of mCMV production in human cells is affected at several levels, which additively or synergistically result in the appearance of species specificity. Hydrolysis of most newly replicated viral DNA and very low capsid protein transcription reduced the potential particle production to insignificant levels. These effects can be ameliorated by adding human cytomegalovirus tegument proteins and immediate-early protein 1. They function synergistically to produce significant amounts of mCMV in human cells. While the possibility that mouse cytomegalovirus might replicate in human cells raises caution in the use of this virus as a transgene vector, manipulation of the mouse cytomegalovirus genome to allow limited spread to other human cells might also provide an advantage for the distribution of certain transgenic products.
机译:强大的物种特异性和类似的嗜性表明,小鼠巨细胞病毒(mCMV)作为转基因进入人类细胞的潜在载体。我们重新审查了小鼠巨细胞病毒不能在人细胞中高效复制的教条,发现小鼠巨细胞病毒可以产生感染性颗粒,尽管其水平不能维持感染。这一发现表明,小鼠巨细胞病毒可以在人类细胞中经历其生命周期的所有过程,但可能无法很好地适应人类细胞的内在防御。人细胞中mCMV产生的抑制在几个水平上受到影响,这加在一起或协同作用导致出现物种特异性。大部分新复制的病毒DNA的水解和衣壳蛋白的极低转录将潜在的颗粒产生降低到微不足道的水平。通过添加人巨细胞病毒外皮蛋白和即早蛋白质1可以改善这些作用。它们协同作用,在人细胞中产生大量的mCMV。尽管小鼠巨细胞病毒可能在人细胞中复制的可能性提高了使用该病毒作为转基因载体的警惕性,但操纵小鼠巨细胞病毒基因组以使其有限地传播到其他人细胞中,也可能为某些转基因产物的分布提供了优势。 。

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