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牛白血病病毒在体内早期感染期间获得的外周血细胞中的转录。

Transcription of bovine leukemia virus in peripheral blood cells obtained during early infection in vivo.

作者信息

Radke K, Sigala T J, Grossman D

机构信息

Department of Avian Sciences, University of California, Davis 95616-8532.

出版信息

Microb Pathog. 1992 May;12(5):319-31. doi: 10.1016/0882-4010(92)90095-6.

DOI:10.1016/0882-4010(92)90095-6
PMID:1323740
Abstract

Bovine leukemia virus (BLV) is transcriptionally silent in most circulating peripheral blood mononuclear cells (PBMCs) of animals with well-established infections. Using PBMCs from a newly infected sheep, we asked whether viral transcription proceeded differently during the initial months of infection, when the prevalence of BLV-infected cells and the host's immunological response change markedly. Shortly after being injected with BLV, the animal displayed a characteristic, transient increase in PBMCs that transcribed BLV when cultured. Even when transcriptionally competent PBMCs were most prevalent (1.2%), only rare cells in the circulation (1 in 50,000) contained enough BLV transcripts to be identified readily by in situ hybridization. However, at one point several weeks later, some PBMCs appeared to contain small amounts of BLV RNA as soon as they had been purified from blood. Throughout this period, BLV-transcribing PBMCs greatly outnumbered virus-producing cells, which were counted using a new infectious centers assay. Its viscous medium reduced cell to cell contact among PBMCs, enabling increased detection of BLV-producing cells at a time when virus-specific killer cells might be active. Early infection was polyclonal, and most infected PBMCs transcribed BLV upon being cultured. By 2 months after infection, provirus-containing cells were as abundant as they had been earlier, but few cells transcribed BLV. These results suggest that BLV-infected cells are more easily stimulated to transcribe the provirus and produce infectious virus during the early months of a new infection.

摘要

在感染已确立的动物的大多数循环外周血单核细胞(PBMC)中,牛白血病病毒(BLV)转录沉默。我们使用来自一只新感染绵羊的PBMC,研究在感染的最初几个月,当BLV感染细胞的患病率和宿主的免疫反应发生显著变化时,病毒转录是否会有不同的进展。在注射BLV后不久,该动物的PBMC出现了特征性的短暂增加,这些PBMC在培养时会转录BLV。即使转录活性PBMC最为普遍(1.2%)时,循环中也只有极少数细胞(50000个中有1个)含有足够的BLV转录本,能够通过原位杂交轻易鉴定出来。然而,在几周后的某个时间点,一些PBMC从血液中纯化出来后似乎就含有少量的BLV RNA。在整个这段时间里,转录BLV的PBMC数量远远超过产生病毒的细胞,后者是使用一种新的感染中心检测法计数的。其粘性培养基减少了PBMC之间的细胞间接触,在病毒特异性杀伤细胞可能活跃的时候,能够增加对产生BLV细胞的检测。早期感染是多克隆的,大多数受感染的PBMC在培养时会转录BLV。感染后2个月,含前病毒的细胞数量与早期一样多,但很少有细胞转录BLV。这些结果表明,在新感染的最初几个月,受BLV感染的细胞更容易被刺激转录前病毒并产生感染性病毒。

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