CCR4 expression on host T cells is a driver for alloreactive responses and lung rejection
Vyacheslav Palchevskiy, Ying Ying Xue, Rita Kern, Stephen S. Weigt, Aric L. Gregson, Sophie X. Song, Michael C. Fishbein, Cory M. Hogaboam, David M. Sayah, Joseph P. Lynch III, Michael P. Keane, David G. Brooks, John A. Belperio
Vyacheslav Palchevskiy, Ying Ying Xue, Rita Kern, Stephen S. Weigt, Aric L. Gregson, Sophie X. Song, Michael C. Fishbein, Cory M. Hogaboam, David M. Sayah, Joseph P. Lynch III, Michael P. Keane, David G. Brooks, John A. Belperio
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Research Article Immunology Transplantation

CCR4 expression on host T cells is a driver for alloreactive responses and lung rejection

Abstract

Despite current immunosuppressive strategies, long-term lung transplant outcomes remain poor due to rapid allogenic responses. Using a stringent mouse model of allo-airway transplantation, we identified the CCR4-ligand axis as a central node driving secondary lymphoid tissue homing and activation of the allogeneic T cells that prevent long-term allograft survival. CCR4 deficiency on transplant recipient T cells diminished allograft injury and when combined with CTLA4-Ig led to lung allograft accommodation lasting longer than in any previous study to our knowledge. Thus, we identify CCR4-ligand interactions as a central mechanism driving allogeneic transplant rejection and suggest it as a potential target to enhance long-term lung transplant survival.

Authors

Vyacheslav Palchevskiy, Ying Ying Xue, Rita Kern, Stephen S. Weigt, Aric L. Gregson, Sophie X. Song, Michael C. Fishbein, Cory M. Hogaboam, David M. Sayah, Joseph P. Lynch III, Michael P. Keane, David G. Brooks, John A. Belperio

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Figure 5

CCR4–/– recipients have a reduction in airway allograft–infiltrating cytotoxic lymphocytes and their mediators.

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CCR4–/– recipients have a reduction in airway allograft–infiltrating cyt...
Day 7 whole airway allografts from CCR4–/– and CCR4+/+ recipients were analyzed for allograft-infiltrating T cell subpopulations and cytotoxic mediators using flow cytometry, Luminex, and qPCR. (A and B) Frequency of allograft-infiltrating CD4+ and CD8+ T cells as well as their subpopulations. (CE) Whole allograft homogenates protein concentrations for IL-2, TNF-α, and IFN-γ. (F–H) Whole allograft homogenate mRNA expression of FasL, perforin 1, and Foxp3. Data are representative of 4–7 mice per group. Error bars indicate SEM. Significance was determined by Mann-Whitney U test; *P < 0.05.