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Generation of a replication-competent chimeric simian-human immunodeficiency virus carrying env from subtype C clinical isolate through intracellular homologous recombination.

机译:通过细胞内同源重组从C型亚型临床分离株中产生带有env的具有复制能力的嵌合猿猴-人免疫缺陷病毒。

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摘要

A new simian-human immunodeficiency virus (SHIV), carrying env from an uncloned HIV-1 subtype C clinical isolate (97ZA012), was generated through intracellular homologous recombination, a DNA repair mechanism of the host cell. PCR fragments amplified from an existing SHIV plasmid (a 7-kb fragment from the 5' end and a 1.5-kb fragment from the 3' end) and a 4-kb fragment amplified from 97ZA012 cDNA containing env were co-transfected to human lymphoid cells. The resulting recombinant was subjected to serial passage in rhesus peripheral blood mononuclear cells (RhPBMCs). The resulting SHIV 97ZA012 was replication competent in RhPBMCs and monkey alveolar macrophages, and possessed CCR5 preference as an entry co-receptor. Experimental infection of rhesus macaques with SHIV 97ZA012 caused high titers of plasma viremia and a transient but profound depletion of CD4(+) T lymphocytes in the lung. Animal-to-animal passage was shown to be a promising measure for further adaptation of the virus in monkeys.
机译:通过细胞内同源重组(一种宿主细胞的DNA修复机制),产生了一种新的猿人免疫缺陷病毒(SHIV),其携带来自未克隆的HIV-1 C型亚临床分离株(97ZA012)的env。从现有SHIV质粒扩增的PCR片段(从5'端开始的7 kb片段和从3'端开始的1.5 kb片段)和从包含env的97ZA012 cDNA扩增的4 kb片段被共转染人淋巴样细胞。将所得重组体在恒河猴外周血单核细胞(RhPBMC)中进行连续传代。所得的SHIV 97ZA012在RhPBMC和猴肺泡巨噬细胞中具有复制能力,并具有CCR5偏好作为进入共受体。用SHIV 97ZA012进行的恒河猴的实验性感染导致高滴度的血浆病毒血症以及肺中CD4(+)T淋巴细胞的短暂但深度耗竭。动物到动物的传代被证明是该病毒在猴子中进一步适应的有前途的措施。

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