Literature DB >> 22711904

Antiviral inhibitory capacity of CD8+ T cells predicts the rate of CD4+ T-cell decline in HIV-1 infection.

Hongbing Yang1, Hao Wu, Gemma Hancock, Genevieve Clutton, Nellia Sande, Xiaoning Xu, Huiping Yan, Xiaojie Huang, Brian Angus, Kristin Kuldanek, Sarah Fidler, Thomas N Denny, Jacqueline Birks, Andrew McMichael, Lucy Dorrell.   

Abstract

BACKGROUND: Rare human immunodeficiency virus type 1 (HIV-1)-infected individuals who maintain control of viremia without therapy show potent CD8+ T-cell-mediated suppression of viral replication in vitro. Whether this is a determinant of the rate of disease progression in viremic individuals is unknown.
METHODS: We measured CD8+ T-cell-mediated inhibition of a heterologous HIV-1 isolate in 50 HIV-1-seropositive adults with diverse progression rates. Linear mixed models were used to determine whether CD8+ T-cell function could explain variation in the rate of CD4+ T-cell decline.
RESULTS: There was a significant interaction between CD8+ T-cell antiviral activity in vitro and the rate of CD4+ T-cell decline in chronically infected individuals (P < .0001). In a second prospective analysis of recently infected subjects followed for up to 3 years, CD8+ T-cell antiviral activity strongly predicted subsequent CD4+ T-cell decline (P < .0001) and explained up to 73% of the interindividual variation in the CD4+ T-cell slope. In addition, it was inversely associated with viral load set point (r = -0.68 and P = .002).
CONCLUSIONS: The antiviral inhibitory capacity of CD8+ T cells is highly predictive of CD4+ T-cell loss in early HIV-1 infection. It has potential as a benchmark of effective immunity in vaccine evaluation.

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Year:  2012        PMID: 22711904      PMCID: PMC4192045          DOI: 10.1093/infdis/jis379

Source DB:  PubMed          Journal:  J Infect Dis        ISSN: 0022-1899            Impact factor:   5.226


  42 in total

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6.  Predictive value of plasma HIV RNA level on rate of CD4 T-cell decline in untreated HIV infection.

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6.  Inhibitory potential of subpopulations of CD8+ T cells in HIV-1-infected elite suppressors.

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7.  Comment on clinical development of candidate HIV vaccines: different problems for different vaccines.

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