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Construction of a High Titer Infectious HIV-1 Subtype C Proviral Clone from South Africa

机译:南非高滴度感染性HIV-1 C型亚型原病毒克隆的构建

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The Human Immunodeficiency Virus type 1 (HIV-1) subtype C is currently the predominant subtype worldwide. Cell culture studies of Sub-Saharan African subtype C proviral plasmids are hampered by the low replication capacity of the resulting viruses, although viral loads in subtype C infected patients are as high as those from patients with subtype B. Here, we describe the sequencing and construction of a new HIV-1 subtype C proviral clone (pZAC), replicating more than one order of magnitude better than the previous subtype C plasmids. We identify the env-region for being the determinant for the higher viral titers and the pZAC Env to be M-tropic. This higher replication capacity does not lead to a higher cytotoxicity compared to previously described subtype C viruses. In addition, the pZAC Vpu is also shown to be able to down-regulate CD4, but fails to fully counteract CD317.
机译:目前,人类免疫缺陷病毒1型(HIV-1)C亚型是全球主要亚型。撒哈拉以南非洲C型前病毒质粒的细胞培养研究由于所得病毒的低复制能力而受到阻碍,尽管C型感染患者的病毒载量与B型患者的病毒载量一样高。在这里,我们描述了测序和新的HIV-1 C型亚型原病毒克隆(pZAC)的构建,其复制能力比以前的C型亚型质粒高一个数量级。我们确定env-区域是较高病毒滴度的决定因素,而pZAC Env是M-向性的。与先前描述的C型亚型病毒相比,这种较高的复制能力不会导致较高的细胞毒性。另外,pZAC Vpu还显示出能够下调CD4,但不能完全抵消CD317。

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