Immune evasion activities of accessory proteins Vpu, Nef and Vif are conserved in acute and chronic HIV-1 infection

辅助蛋白 Vpu、Nef 和 Vif 的免疫逃避活性在急性和慢性 HIV-1 感染中得到保留

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作者:Petra Mlcochova, Luis Apolonia, Silvia F Kluge, Aishwarya Sridharan, Frank Kirchhoff, Michael H Malim, Daniel Sauter, Ravindra K Gupta

Abstract

Heterosexual HIV-1 transmission has been identified as a genetic bottleneck and a single transmitted/founder (T/F) variant with reduced sensitivity to type I interferon initiates productive infection in most cases. We hypothesized that particularly active accessory protein(s) may confer T/F viruses with a selective advantage in establishing HIV infection. Thus, we tested vpu, vif and nef alleles from six T/F and six chronic (CC) viruses in assays for 9 immune evasion activities involving the counteraction of interferon-stimulated genes and modulation of ligands known to activate innate immune cells. All functions were highly conserved with no significant differences between T/F and CC viruses, suggesting that these accessory protein functions are important throughout the course of infection.

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