CD8 apoptosis may be a predictor of T cell number normalization after immune reconstitution in HIV

BACKGROUND: As part of the Houston Vanguard study, a subset of 10 patients randomized to receive IL-2 therapy were compared to 4 patients randomized to not receive IL-2, for markers of T cell activation and death during the first three cycles of IL-2. All patients were treated with combination antir...

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Detalles Bibliográficos
Autores principales: Lewis, Dorothy E, Gross, Kimber L, Diez, Martine M, Martinez, Maria L, Lukefahr, Helen N, Kozinetz, Claudia A, Arduino, Roberto C
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2007
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1800849/
https://www.ncbi.nlm.nih.gov/pubmed/17263884
http://dx.doi.org/10.1186/1479-5876-5-9
Descripción
Sumario:BACKGROUND: As part of the Houston Vanguard study, a subset of 10 patients randomized to receive IL-2 therapy were compared to 4 patients randomized to not receive IL-2, for markers of T cell activation and death during the first three cycles of IL-2. All patients were treated with combination antiretroviral therapy (ART) and were virally suppressed. The purpose of the study was to examine the role of CD8+ T cell death in responses to ART and IL-2 therapy. METHODS: Lymphocytes were examined at Day 0, 5 and 30 days during three cycles of IL-2 therapy. CD25, CD38, HLA-DR expression and annexin (cell death) were examined on CD4 and CD8 subpopulations. Follow up studies examined CD4 levels and CD4:CD8 reconstitution after 6 years using both univariant and multivariate analyses. RESULTS: Human lymphocytes responded to IL-2 therapy by upregulation of CD25 on CD4(+ )T cells, leading to an increase in CD4 cell counts. CD8(+ )T cells did not increase CD25 expression, but upregulated activation antigens (CD38 and DR) and had increased death. At baseline, 7 of the 14 patients had high CD8(+ )T cell apoptosis (mean 17.0% ± 6.0). We did an exploratory analysis of immune status after six years, and found that baseline CD8(+ )T cell apoptosis was correlated with CD4 cell count gain beginning two years post enrollment. Patients with low levels of CD8(+ )T cell apoptosis at baseline (mean 2.2% ± 2.1) had significantly higher CD4 cell counts and more normalized CD4:CD8 ratios than patients with high CD8(+ )T cell apoptosis (mean CD4 cell counts 1,209 ± 164 vs 754 ± 320 cells/mm(3); CD4:CD8 ratios 1.55 vs. 0.70, respectively). CONCLUSION: We postulate that CD8(+ )T cell apoptosis may reflect inherent activation status, which continues in some patients even though viral replication is suppressed which influences the ability of CD4(+ )T cells to rebound. Levels of CD8(+ )T cell apoptosis may therefore be an independent predictor of immune status, which should be shown in a prospective study.

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