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Molecular identification cloning and characterization of transmitted/founder HIV-1 subtype A D and A/D infectious molecular clones

机译:透射/创始人HIV-1亚型AD和A / D感染分子克隆的分子鉴定克隆和表征

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摘要

We report the molecular identification, cloning and initial biological characterization of 12 full-length HIV-1 subtype A, D and A/D recombinant transmitted/founder (T/F) genomes. T/F genomes contained intact canonical open reading frames and all T/F viruses were replication competent in primary human T-cells, although subtype D virus replication was more efficient (p<0.05). All 12 viruses utilized CCR5 but not CXCR4 as a co-receptor for entry and exhibited a neutralization profile typical of tier 2 primary virus strains, with significant differences observed between subtype A and D viruses with respect to sensitivity to monoclonal antibodies VRC01, PG9 and PG16 and polyclonal subtype C anti-HIV IgG (p<0.05 for each). The present report doubles the number of T/F HIV-1 clones available for pathogenesis and vaccine research and extends their representation to include subtypes A, B, C and D.
机译:我们报告了分子鉴定,克隆和12全长HIV-1亚型A,D和A / D重组传播/奠基人(T / F)基因组的初始生物学特性。 T / F基因组包含完整的规范开放阅读框,并且所有T / F病毒在原代人T细胞中均具有复制能力,尽管D型亚型病毒复制更为有效(p <0.05)。所有12种病毒均使用CCR5而非CXCR4作为进入的共受体,并表现出典型的第2层一级病毒株的中和谱,在亚型和D型病毒之间对单克隆抗体VRC01,PG9和PG16的敏感性方面观察到显着差异和多克隆C型亚型抗HIV IgG(每种p <0.05)。本报告使可用于发病机理和疫苗研究的T / F HIV-1克隆数量翻了一番,并将其代表范围扩大到包括亚型A,B,C和D。

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