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Replication competent virus as an important source of bias in HIV latency models utilizing single round viral constructs

机译:复制有效病毒是利用单轮病毒构建体在HIV潜伏期模型中产生偏见的重要来源

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摘要

The central memory T cell (TCM) model forms a unique HIV-1 latency model based on primary cells that closely resemble in vivo TCM. The virus employed in this model is based on an engineered vector incapable of replication after initial infection. We show that despite this strategy, replication competent viral particles are released into the culture medium due to recombination between overlapping sequences of the env deleted HIV genome that is co-transfected with intact env. This finding emphasizes the need for careful data analysis and interpretation if similar constructs are employed and urges for additional caution during laboratory work.Electronic supplementary materialThe online version of this article (doi:10.1186/s12977-014-0070-3) contains supplementary material, which is available to authorized users.
机译:中央记忆T细胞(TCM)模型基于与体内TCM非常相似的原代细胞形成独特的HIV-1潜伏期模型。该模型中使用的病毒基于工程载体,该载体在初次感染后无法复制。我们显示,尽管采取了这种策略,但由于与完整的env共转染的env缺失的HIV基因组的重叠序列之间的重组,使具有复制能力的病毒颗粒被释放到培养基中。这一发现强调了如果采用类似的结构,则需要进行仔细的数据分析和解释,并敦促在实验室工作中更加谨慎。电子补充材料本文的在线版本(doi:10.1186 / s12977-014-0070-3)包含补充材料,可供授权用户使用。

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