R A Picking scite author profile

mediated virus inhibition than cognate T/F viruses, demonstrating that the virus escapes early from CD8؉ T cell-mediated inhibition of virus replication. CD8 ؉ T cell antigen-specific subsets mediated inhibition of T/F virus replication via soluble components, and these soluble responses were stimulated by peptide pools that include epitopes that were shown to drive HIV-1 escape during AHI. These data provide insights into the mechanisms of CD8-mediated virus inhibition and suggest that functional analyses will be important for determining whether similar antigen-specific virus inhibition can be induced by T cell-directed vaccine strategies.

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CD4+CD8+ T Cells Represent a Significant Portion of the Anti-HIV T Cell Response to Acute HIV Infection

Frahm

Picking

Kuruc

et al. 2012

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Previous studies have revealed that HIV-infected individuals possess circulating CD4+CD8+ double-positive (DP) T cells specific for HIV Ags. In the present study, we analyzed the proliferation and functional profile of circulating DP T cells from 30 acutely HIV-infected individuals and 10 chronically HIV-infected viral controllers. The acutely infected group had DP T cells that showed more proliferative capability and multifunctionality than did both their CD4+ and CD8+ T cells. DP T cells were found to exhibit greater proliferation and higher multifunctionality compared with CD4 T cells in the viral controller group. The DP T cell response represented 16% of the total anti-HIV proliferative response and >70% of the anti-HIV multifunctional response in the acutely infected subjects. Proliferating DP T cells of the acutely infected subjects responded to all HIV Ag pools with equal magnitude. Conversely, the multifunctional response was focused on the pool representing Nef, Rev, Tat, VPR, and VPU. Meanwhile, the controllers’ DP T cells focused on Gag and the Nef, Rev, Tat, VPR, and VPU pool for both their proliferative and multifunctional responses. Finally, we show that the presence of proliferating DP T cells following all HIV Ag stimulations is well correlated with proliferating CD4 T cells whereas multifunctionality appears to be largely independent of multifunctionality in other T cell compartments. Therefore, DP T cells represent a highly reactive cell population during acute HIV infection, which responds independently from the traditional T cell compartments.

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The role of inhibition of pyruvate kinase in the stimulation of gluconeogenesis by glucagon: A reevaluation

Haynes

Picking

1990

Archives of Biochemistry and Biophysics

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R A Picking

Initial HIV-1 Antigen-Specific CD8 ⁺ T Cells in Acute HIV-1 Infection Inhibit Transmitted/Founder Virus Replication

CD4+CD8+ T Cells Represent a Significant Portion of the Anti-HIV T Cell Response to Acute HIV Infection

The role of inhibition of pyruvate kinase in the stimulation of gluconeogenesis by glucagon: A reevaluation

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R A Picking

Initial HIV-1 Antigen-Specific CD8 + T Cells in Acute HIV-1 Infection Inhibit Transmitted/Founder Virus Replication

CD4+CD8+ T Cells Represent a Significant Portion of the Anti-HIV T Cell Response to Acute HIV Infection

The role of inhibition of pyruvate kinase in the stimulation of gluconeogenesis by glucagon: A reevaluation

Contact Info

Product

Resources

About

Initial HIV-1 Antigen-Specific CD8 ⁺ T Cells in Acute HIV-1 Infection Inhibit Transmitted/Founder Virus Replication