• Am. J. Respir. Crit. Care Med. · Jan 2016

    Polyfunctional T cell Responses Predict Protection from Cytomegalovirus After Lung Transplant.

    • Laurie D Snyder, Cliburn Chan, Darongsae Kwon, John S Yi, Jessica A Martissa, C Ashley Finlen Copeland, Robyn J Osborne, Sara D Sparks, Scott M Palmer, and Kent J Weinhold.
    • 1 Department of Medicine.
    • Am. J. Respir. Crit. Care Med. 2016 Jan 1; 193 (1): 78-85.

    RationaleCytomegalovirus (CMV), which is one of the most common infections after lung transplantation, is associated with chronic lung allograft dysfunction and worse post-transplantation survival. Current approaches for at-risk patients include a fixed duration of antiviral prophylaxis despite the associated cost and side effects.ObjectivesWe sought to identify a specific immunologic signature that predicted protection from subsequent CMV.MethodsCMV-seropositive lung transplantation recipients were included in the discovery (n = 43) and validation (n = 28) cohorts. Polyfunctional CMV-specific immunity was assessed by stimulating peripheral blood mononuclear cells with CMV pp65 or IE-1 peptide pools and then by measuring T-cell expression of CD107a, IFN-γ, tumor necrosis factor-α (TNF-α), and IL-2. Recipients were prospectively monitored for subsequent viremia. A Cox proportional hazards regression model that considered cytokine responses individually and in combination was used to create a predictive model for protection from CMV reactivation. This model was then applied to the validation cohort.Measurements And Main ResultsUsing the discovery cohort, we identified a specific combination of polyfunctional T-cell subsets to pp65 that predicted protection from subsequent CMV viremia (concordance index 0.88 [SE, 0.087]). The model included both protective (CD107a(-)/IFN-γ(+)/IL-2(+)/TNF-α(+) CD4(+) T cells, CD107a(-)/IFN-γ(+)/IL-2(+)/TNF-α(+) CD8(+) T cells) and detrimental (CD107a(+)/IFN-γ(+)/IL-2(-)/TNF-α(-) CD8(+) T cells) subsets. The model was robust in the validation cohort (concordance index 0.81 [SE, 0.103]).ConclusionsWe identified and validated a specific T-cell polyfunctional response to CMV antigen stimulation that provides a clinically useful prediction of subsequent cytomegalovirus risk. This novel diagnostic approach could inform the optimal duration of individual prophylaxis.

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