Non-self recognition by monocytes initiates allograft rejection
Martin H. Oberbarnscheidt, … , David M. Rothstein, Fadi G. Lakkis
Martin H. Oberbarnscheidt, … , David M. Rothstein, Fadi G. Lakkis
Published July 1, 2014
Citation Information: J Clin Invest. 2014;124(8):3579-3589. https://doi.org/10.1172/JCI74370.
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Non-self recognition by monocytes initiates allograft rejection

Abstract

Maturation of T cell–activating APCs directly links innate and adaptive immunity and is typically triggered by microbial infection. Transplantation of allografts, which are sterile, generates strong T cell responses; however, it is unclear how grafts induce APC maturation in the absence of microbial-derived signals. A widely accepted hypothesis is that dying cells in the graft release “danger” molecules that induce APC maturation and initiate the adaptive alloimmune response. Here, we demonstrated that danger signals associated with dying cells are not sufficient to initiate alloimmunity, but that recognition of allogeneic non-self by the innate immune system is required. In WT as well as in T cell–, B cell–, and innate lymphoid cell–deficient mice, allogeneic grafts elicited persistent differentiation of monocytes into mature DCs that expressed IL-12 and stimulated T cell proliferation and IFN-γ production. In contrast, syngeneic grafts in the same mice elicited transient and less pronounced differentiation of monocytes into DCs, which neither expressed IL-12 nor stimulated IFN-γ production. In a model in which T cell recognition is restricted to a single foreign antigen on the graft, rejection occurred only if the allogeneic non-self signal was also sensed by the host’s innate immune system. These findings underscore the importance of innate recognition of allogeneic non-self by monocytes in initiating graft rejection.

Authors

Martin H. Oberbarnscheidt, Qiang Zeng, Qi Li, Hehua Dai, Amanda L. Williams, Warren D. Shlomchik, David M. Rothstein, Fadi G. Lakkis

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Figure 6

Innate sensing of allogeneic non-self precipitates graft rejection.

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Innate sensing of allogeneic non-self precipitates graft rejection. (A) ...
(A) Heart grafts from multiple donor strains (shown on x axis) were transplanted into B6 RAG–/–γc–/–CX3CR1gfp/+ recipients, and host-derived mature mono-DCs present in the grafts were enumerated by flow cytometry 3 days later. (B and C) Graft recipients, as in A, received 5 × 105 OT-II cells 2 days after transplantation. Grafts and spleens were harvested on the day of rejection or at termination of the experiment (day 42). IFN-γ production by OT-II cells in the spleen is shown in B. Allograft survival, number of graft-infiltrating T cells, and representative graft sections stained with anti-CD3 (red) and hematoxylin (blue) are shown in C (original magnification, ×2). *P < 0.05 compared with B6 and B6-OVA groups.