首页> 美国卫生研究院文献>Journal of Virology >Phenotypic and Genotypic Comparisons of CCR5- and CXCR4-Tropic Human Immunodeficiency Virus Type 1 Biological Clones Isolated from Subtype C-Infected Individuals
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Phenotypic and Genotypic Comparisons of CCR5- and CXCR4-Tropic Human Immunodeficiency Virus Type 1 Biological Clones Isolated from Subtype C-Infected Individuals

机译:从C型亚型感染个体中分离出的CCR5-和CXCR4-热带人类免疫缺陷病毒1型生物学克隆的表型和基因型比较

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摘要

Individuals infected with human immunodeficiency virus type 1 (HIV-1) subtype C infrequently harbour X4 viruses. We studied R5 and X4 biological clones generated from HIV-1 subtype C-infected individuals. All subtype C R5 viruses demonstrated slower profiles of replication on CD4+ lymphocytes in comparison to subtype B viruses, whereas subtype C X4 viruses replicated with comparable efficiency to subtype B X4 viruses. No differences were identified in CC or CXC chemokine inhibitions (RANTES and SDF-1α, respectively) between subtype C and subtype B viruses. Immature dendritic cells were shown in coculture experiments to similarly enhance the infection of subtype C and subtype B R5 as well as X4 viruses. By amino acid sequence analysis, we showed that the R5 and X4 subtype C gp120 envelope gene alterations were similar to those for a switching subtype B virus, specifically with respect to the V3 charge and envelope N-linked glycosylation patterns. By phylogenetic analysis, we showed that one patient was infected with HIV-1 C′ and the other was infected with HIV-1 C" and that one of the patients harbored a virus that was a recombinant in the gp120 env gene between an R5 and an X4 virus, with the resultant virus being R5. No differences were identified between the long terminal repeat regions of the subtype C R5 and X4 biological clones. These results indicate that even though R5 subtype C viruses are restrictive for virus replication, the R5-to-X4 phenotype switch can occur and does so in a manner similar to that of subtype B viruses.
机译:感染了人类免疫缺陷病毒1型(HIV-1)C亚型的个体很少携带X4病毒。我们研究了从HIV-1亚型C感染个体产生的R5和X4生物克隆。与B型亚型病毒相比,所有C R5型亚型病毒在CD4 + 淋巴细胞上的复制速度均较慢,而C X4型亚型病毒的复制效率与B X4型亚种病毒相当。 C型和B型病毒之间的CC或CXC趋化因子抑制作用(分别为RANTES和SDF-1α)没有差异。共培养实验显示未成熟的树突状细胞可类似地增强C亚型和B R5亚型以及X4病毒的感染。通过氨基酸序列分析,我们发现R5和X4 C亚型gp120包膜基因的改变与转换亚型B病毒的改变相似,特别是在V3电荷和N联糖基化模式方面。通过系统发育分析,我们显示一名患者感染了HIV-1 C',另一名患者感染了HIV-1 C“,其中一名患者携带了一种病毒,该病毒在R5和X4病毒,其最终病毒为R5。在C5亚型R5和X4生物克隆的长末端重复区域之间没有发现差异,这些结果表明,即使C5 R5亚型限制病毒复制,R5- to-X4表型转换可以发生,并且以类似于B型亚型病毒的方式发生。

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