Central memory CD8+ T lymphocytes mediate lung allograft acceptance
Alexander Sasha Krupnick, … , Andrew E. Gelman, Daniel Kreisel
Alexander Sasha Krupnick, … , Andrew E. Gelman, Daniel Kreisel
Published February 24, 2014
Citation Information: J Clin Invest. 2014;124(3):1130-1143. https://doi.org/10.1172/JCI71359.
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Research Article

Central memory CD8+ T lymphocytes mediate lung allograft acceptance

Abstract

Memory T lymphocytes are commonly viewed as a major barrier for long-term survival of organ allografts and are thought to accelerate rejection responses due to their rapid infiltration into allografts, low threshold for activation, and ability to produce inflammatory mediators. Because memory T cells are usually associated with rejection, preclinical protocols have been developed to target this population in transplant recipients. Here, using a murine model, we found that costimulatory blockade–mediated lung allograft acceptance depended on the rapid infiltration of the graft by central memory CD8+ T cells (CD44hiCD62LhiCCR7+). Chemokine receptor signaling and alloantigen recognition were required for trafficking of these memory T cells to lung allografts. Intravital 2-photon imaging revealed that CCR7 expression on CD8+ T cells was critical for formation of stable synapses with antigen-presenting cells, resulting in IFN-γ production, which induced NO and downregulated alloimmune responses. Thus, we describe a critical role for CD8+ central memory T cells in lung allograft acceptance and highlight the need for tailored approaches for tolerance induction in the lung.

Authors

Alexander Sasha Krupnick, Xue Lin, Wenjun Li, Ryuiji Higashikubo, Bernd H. Zinselmeyer, Hollyce Hartzler, Kelsey Toth, Jon H. Ritter, Mikhail Y. Berezin, Steven T. Wang, Mark J. Miller, Andrew E. Gelman, Daniel Kreisel

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Figure 9

Chemokine receptor expression regulates CD8+ T cell–mediated lung acceptance.

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Chemokine receptor expression regulates CD8+ T cell–mediated lung accept...
(A) Graft infiltration by PTX-treated or untreated anti-donor (BALB/c) central memory, anti–third party (CBA/Ca) central memory, or anti-donor (BALB/c) effector memory B6 CD8+CD45.1+ T cells (comparison within each group by unpaired t test). (B) Injection of Ccr7–/– CD8+ T cells does not restore allograft acceptance in B6 Cd8–/– recipients (P = 0.00054 vs. Figure 2E by Mantel-Haenszel χ2 test). The arrow points to perivascular infiltrates. (C) Immunosuppressed BALB/c→B6 Cd8–/– recipients reconstituted with wild-type B6 CD8+ T cells (n = 8) had higher graft Ifng levels than those reconstituted with B6 Ccr7–/– CD8+ T cells (n = 5) (day 4) (unpaired t test). (D) Majority of recipient-derived graft-infiltrating CD11c+ cells in immunosuppressed BALB/c (CD45.2+)→B6 (CD45.1+) transplants express donor MHC class I (H-2Kd) (n = 3). Numbers in top density plot represent percentages of CD11c+ cells expressing CD45.1 (recipient) vs. CD45.2 (donor). Numbers in bottom density plot represent percentages of recipient CD45.1+CD45.2CD11c+ cells expressing donor (H-2Kd) vs. recipient (H-2Kb) MHC class I. Representative of 3 independent experiments. All gross and histological appearances as well as rejection grades represent grafts at 7 days after transplantation (original magnification, ×200 [histology, H&E staining]).