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Human Cytomegalovirus Manipulation of Latently Infected Cells

机译:人类巨细胞病毒对潜伏感染细胞的操纵

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摘要

Primary infection with human cytomegalovirus (HCMV) results in the establishment of a lifelong infection of the host which is aided by the ability of HCMV to undergo a latent infection. One site of HCMV latency in vivo is in haematopoietic progenitor cells, resident in the bone marrow, with genome carriage and reactivation being restricted to the cells of the myeloid lineage. Until recently, HCMV latency has been considered to be relatively quiescent with the virus being maintained essentially as a “silent partner” until conditions are met that trigger reactivation. However, advances in techniques to study global changes in gene expression have begun to show that HCMV latency is a highly active process which involves expression of specific latency-associated viral gene products which orchestrate major changes in the latently infected cell. These changes are argued to help maintain latent infection and to modulate the cellular environment to the benefit of latent virus. In this review, we will discuss these new findings and how they impact not only on our understanding of the biology of HCMV latency but also how they could provide tantalising glimpses into mechanisms that could become targets for the clearance of latent HCMV.
机译:人巨细胞病毒(HCMV)的初次感染导致建立宿主的终生感染,这是由于HCMV进行潜伏感染的能力所致。体内HCMV潜伏期的一个位点位于骨髓中的造血祖细胞中,而基因组的运输和再激活仅限于髓系的细胞。直到最近,HCMV潜伏期仍被认为相对静止,而该病毒基本上保持为“沉默伴侣”,直到满足触发重新激活的条件为止。但是,研究基因表达的整体变化的技术进步已开始表明,HCMV潜伏期是一个高度活跃的过程,涉及特定的潜伏期相关病毒基因产物的表达,这些产物协调了潜伏感染细胞的主要变化。这些变化被认为有助于维持潜伏感染并调节细胞环境以利于潜伏病毒。在这篇综述中,我们将讨论这些新发现,以及它们不仅会影响我们对HCMV潜伏期生物学的理解,而且还将如何将它们诱人地带入可能成为清除潜在HCMV的目标的机制。

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