Monocytic suppressive cells mediate cardiovascular transplantation tolerance in mice
Mercedes Rodriguez Garcia, … , Jonathan S. Bromberg, Jordi C. Ochando
Mercedes Rodriguez Garcia, … , Jonathan S. Bromberg, Jordi C. Ochando
Published June 14, 2010
Citation Information: J Clin Invest. 2010;120(7):2486-2496. https://doi.org/10.1172/JCI41628.
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Research Article

Monocytic suppressive cells mediate cardiovascular transplantation tolerance in mice

Abstract

One of the main unresolved questions in solid organ transplantation is how to establish indefinite graft survival that is free from long-term treatment with immunosuppressive drugs and chronic rejection (i.e., the establishment of tolerance). The failure to achieve this goal may be related to the difficulty in identifying the phenotype and function of the cell subsets that participate in the induction of tolerance. To address this issue, we investigated the suppressive roles of recipient myeloid cells that may be manipulated to induce tolerance to transplanted hearts in mice. Using depleting mAbs, clodronate-loaded liposomes, and transgenic mice specific for depletion of CD11c+, CD11b+, or CD115+ cells, we identified a tolerogenic role for CD11b+CD115+Gr1+ monocytes during the induction of tolerance by costimulatory blockade with CD40L-specific mAb. Early after transplantation, Gr1+ monocytes migrated from the bone marrow into the transplanted organ, where they prevented the initiation of adaptive immune responses that lead to allograft rejection and participated in the development of Tregs. Our results suggest that mobilization of bone marrow CD11b+CD115+Gr1+ monocytes under sterile inflammatory conditions mediates the induction of indefinite allograft survival. We propose that manipulating the common bone marrow monocyte progenitor could be a useful clinical therapeutic approach for inducing transplantation tolerance.

Authors

Mercedes Rodriguez Garcia, Levi Ledgerwood, Yu Yang, Jiangnan Xu, Girdhari Lal, Bryna Burrell, Ge Ma, Daigo Hashimoto, Yansui Li, Peter Boros, Marcos Grisotto, Nico van Rooijen, Rafael Matesanz, Frank Tacke, Florent Ginhoux, Yaozhong Ding, Shu-Hsia Chen, Gwendalyn Randolph, Miriam Merad, Jonathan S. Bromberg, Jordi C. Ochando

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Figure 1

CD11b+CD115+Gr1+ monocytes are required for tolerance induction to vascularized allografts.

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CD11b+CD115+Gr1+ monocytes are required for tolerance induction to vascu...
(A) Fully allogeneic vascularized cardiac grafts were accepted in tolerogen-treated (DST plus anti-CD40L mAb) CD11c-DTR mice (n = 10), but rejected in tolerogen-treated CD11b-DTR mice (n = 10), after DT administration. (B) Fully allogeneic vascularized cardiac grafts were rejected in tolerogen-treated mice that received the anti-Gr1 mAb RB6-8C5 (n = 10), but accepted in tolerogen-treated mice that received the anti-Gr1 mAb 1A8 (n = 10). Untreated rejecting controls were as in A. (C) Fully allogeneic vascularized cardiac grafts were rejected in tolerogen-treated mice that received clodronate loaded liposomes (clo-lip; n = 10) and in tolerogen-treated MaFIA mice (n = 10) following depletion of CD115-expressing cells. Untreated controls were as in A. Also shown are representative allograft images of H&E staining of the indicated groups at day of rejection or after 100 days of allograft survival. Original magnification, ×40.