Impact of HIV-1 infection and highly active antiretroviral therapy on the kinetics of CD4
            <sup>+</sup>
            and CD8
            <sup>+</sup>
            T cell turnover in HIV-infected patients

Lempicki, Richard A.; Kovacs, Joseph A.; Baseler, Michael; Adelsberger, Joseph W.; Dewar, Robin; Natarajan, Ven; Bosche, Marjorie; Metcalf, Julia A.; Stevens, Randy; Lambert, Laurie; Alvord, W. Gregory; Polis, Michael A.; Davey, Richard T.; Dimitrov, Dimiter S.; Lane, H. Clifford

doi:10.1073/pnas.250472097

Cited by 176 publications

(178 citation statements)

References 25 publications

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“…Although the relative contributions of different cytokines to homeostatic proliferation in humans are difficult to address directly, recent reports are consistent with the view that human and murine T cells have similar requirements [13,14,21,[28][29][30][31][32]. Thus, antigen-independent naive T cell proliferation in the mouse requires TCR tickling, IL-7, and lymphopenia, whereas CD8 memory T cells turn over constitutively, express high levels of the IL-2/ 15Rb chain and require IL-15 or IL-7.…”

Section: Discussionmentioning

confidence: 55%

“…5C) and were also able to consistently reduce the viability of intracellular Mtb (Fig. 5D) [21][22][23]. Cells that pass the G1 cell cycle checkpoint are committed to replicate DNA and complete the cell cycle [22].…”

Section: Generation Of T Emra Cells By Cytokine-stimulated T CM Cellsmentioning

confidence: 84%

“…Cells that pass the G1 cell cycle checkpoint are committed to replicate DNA and complete the cell cycle [22]. The in vivo turnover of T cells can therefore be assessed by ex vivo bromodeoxyuridine (BrdU) incorporation [21]. Freshly purified PBMC from five healthy donors were cultured in the presence of BrdU, and Vc9Vd2 T cells were purified and analyzed for BrdU incorporation in relation to CD27 and CD45RA expression.…”

Section: Generation Of T Emra Cells By Cytokine-stimulated T CM Cellsmentioning

confidence: 99%

“…This assay was carried out by using the procedure reported by Lempicki et al [21]. Vc9Vd2 T cells were isolated by positive selection as described above and incubated with 10 lM BrdU (Sigma) for 4 h at 37 C, 5% CO 2 .…”

Section: Ex Vivo Brdu Labelingmentioning

confidence: 99%

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Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

et al. 2005

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Section: Discussionmentioning

confidence: 55%

Section: Generation Of T Emra Cells By Cytokine-stimulated T CM Cellsmentioning

confidence: 84%

Section: Generation Of T Emra Cells By Cytokine-stimulated T CM Cellsmentioning

confidence: 99%

Section: Ex Vivo Brdu Labelingmentioning

confidence: 99%

See 2 more Smart Citations

Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

et al. 2005

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“…Ex vivo labeling of proliferating naive CD4ϩ T cells was carried out by incubating freshly isolated PBMCs with BrdUrd for 4 h at 37°C as described (11). Labeled cells were analyzed by FACS.…”

Section: Methodsmentioning

confidence: 99%

Increased peripheral expansion of naive CD4+ T cellsin vivoafter IL-2 treatment of patients with HIV infection

Natarajan

Lempicki

Sereti

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

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Intermittent interleukin-2 (IL-2) therapy has been shown to increase the number of CD4؉ T cells, preferentially cells with a naive phenotype, in patients with HIV infection. For this report we investigated the mechanism underlying this expansion by studying the relative roles of peripheral expansion and thymic output. In a cohort of six patients receiving IL-2 over a period of 1 year, the mean number of naive CD4؉ T cells increased from 139 to 387 cells per l while levels of T cell receptor rearrangement excision circles (TRECs) declined from 47,946 to 26,510 copies per 10 6 naive T cells, thus making it unlikely that the CD4؉ T cell count increases were secondary to increase in thymic output. To examine directly the impact of IL-2 on peripheral expansion, peripheral blood mature, naive CD4؉ T cells were labeled ex vivo with 5-bromodeoxyuridine as well as stained directly for Ki67. These studies revealed a 7-fold increase in the percentage of 5-bromodeoxyuridine-positive cells and a 20 -40-fold increase in Ki67 staining in the naive CD4؉ T cell pool in the setting of IL-2 administration. This degree of increase in mature CD4؉ T cell turnover induced by IL-2 does not compromise the future replicative potential of these cells, because longitudinal measurements of telomere length went from 6,981 to 7,153 bp after 1 year of IL-2 therapy. These data strongly suggest that much of the increase in CD4؉ cells associated with IL-2 treatment is caused by peripheral expansion of existing naive CD4؉ T cells rather than increased thymic output and that these increases occur without compromising the potential of these cells for further cell division.

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The CD8⁺HLA‐DR⁺ T cells expanded in HIV‐1 infection are qualitatively identical to those from healthy controls

et al. 2012

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HIV-induced immune activation leads to expansion of a subset of human CD8+ T cells expressing HLA-DR antigens. Expansion of CD8+HLA-DR+ T cells can be also observed in non-HIV settings including several autoimmune diseases and aging. Although these cells are felt to represent “immune exhaustion” and/or to be anergic, their precise role in host defense has remained unclear. Here, we report that this subset of cells exhibits a restricted repertoire, shows evidence of multiple rounds of division, but lacks markers of recent TCR-engagement. Detailed cell cycle analysis revealed that compared with their CD8+HLA-DR-counterpart, the CD8+HLA-DR+ T-cell pool contained an increased fraction of cells in S-phase with elevated levels of the G2/M regulators: cyclin A2, CDC25C, Cdc2 (CDK1), indicating that these cells are not truly anergic but rather experiencing proliferation in vivo. Together, these data support a hypothesis that antigen stimulation leads to the initial expansion of a CD8+ pool of cells in vivo that undergo further expansion independent of ongoing TCR-engagement. No qualitative differences were noted between CD8+HLA-DR+ cells from HIV+ and HIV− donors, indicating that the generation of CD8+HLA-DR+ T cells is a part of normal immune regulation that is exaggerated in the setting of HIV-1 infection.

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Impact of HIV-1 infection and highly active antiretroviral therapy on the kinetics of CD4 ⁺ and CD8 ⁺ T cell turnover in HIV-infected patients

Cited by 176 publications

References 25 publications

Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

Increased peripheral expansion of naive CD4+ T cellsin vivoafter IL-2 treatment of patients with HIV infection

The CD8⁺HLA‐DR⁺ T cells expanded in HIV‐1 infection are qualitatively identical to those from healthy controls

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Impact of HIV-1 infection and highly active antiretroviral therapy on the kinetics of CD4 + and CD8 + T cell turnover in HIV-infected patients

Cited by 176 publications

References 25 publications

Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

Differential requirements for antigen or homeostatic cytokines for proliferation and differentiation of human Vγ9Vδ2 naive, memory and effector T cell subsets

Increased peripheral expansion of naive CD4+ T cellsin vivoafter IL-2 treatment of patients with HIV infection

The CD8+HLA‐DR+ T cells expanded in HIV‐1 infection are qualitatively identical to those from healthy controls

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Impact of HIV-1 infection and highly active antiretroviral therapy on the kinetics of CD4 ⁺ and CD8 ⁺ T cell turnover in HIV-infected patients

The CD8⁺HLA‐DR⁺ T cells expanded in HIV‐1 infection are qualitatively identical to those from healthy controls