Exhaustion of Activated CD8 T Cells Predicts Disease Progression in Primary HIV-1 Infection

Publication

Exhaustion of Activated CD8 T Cells Predicts Disease Progression in Primary HIV-1 Infection

Journal Paper/Review - Jul 14, 2016

Hoffmann Matthias, Frater John, Phillips Rodney, Fidler Sarah, Fox Julie, Nwokolo Nneka, Weber Jonathan, Babiker Abdel, Kinloch Sabine, Fisher Martin, Brown Helen, Robinson Nicola, Willberg Christian B, Meyerowitz Jodi, Hurst Jacob, Hickling Stephen, Martin Genevieve E, Pantazis Nikos

Citation

Hoffmann M, Frater J, Phillips R, Fidler S, Fox J, Nwokolo N, Weber J, Babiker A, Kinloch S, Fisher M, Brown H, Robinson N, Willberg C, Meyerowitz J, Hurst J, Hickling S, Martin G, Pantazis N. Exhaustion of Activated CD8 T Cells Predicts Disease Progression in Primary HIV-1 Infection. PLoS Pathog 2016; 12:e1005661.

Type

Journal Paper/Review (English)

Journal

PLoS Pathog 2016; 12

Publication Date

Jul 14, 2016

Issn Electronic

1553-7374

Pages

e1005661

Brief description/objective

The rate at which HIV-1 infected individuals progress to AIDS is highly variable and impacted by T cell immunity. CD8 T cell inhibitory molecules are up-regulated in HIV-1 infection and associate with immune dysfunction. We evaluated participants (n = 122) recruited to the SPARTAC randomised clinical trial to determine whether CD8 T cell exhaustion markers PD-1, Lag-3 and Tim-3 were associated with immune activation and disease progression. Expression of PD-1, Tim-3, Lag-3 and CD38 on CD8 T cells from the closest pre-therapy time-point to seroconversion was measured by flow cytometry, and correlated with surrogate markers of HIV-1 disease (HIV-1 plasma viral load (pVL) and CD4 T cell count) and the trial endpoint (time to CD4 count <350 cells/μl or initiation of antiretroviral therapy). To explore the functional significance of these markers, co-expression of Eomes, T-bet and CD39 was assessed. Expression of PD-1 on CD8 and CD38 CD8 T cells correlated with pVL and CD4 count at baseline, and predicted time to the trial endpoint. Lag-3 expression was associated with pVL but not CD4 count. For all exhaustion markers, expression of CD38 on CD8 T cells increased the strength of associations. In Cox models, progression to the trial endpoint was most marked for PD-1/CD38 co-expressing cells, with evidence for a stronger effect within 12 weeks from confirmed diagnosis of PHI. The effect of PD-1 and Lag-3 expression on CD8 T cells retained statistical significance in Cox proportional hazards models including antiretroviral therapy and CD4 count, but not pVL as co-variants. Expression of 'exhaustion' or 'immune checkpoint' markers in early HIV-1 infection is associated with clinical progression and is impacted by immune activation and the duration of infection. New markers to identify exhausted T cells and novel interventions to reverse exhaustion may inform the development of novel immunotherapeutic approaches.