Linking erythropoietin to Treg-dependent allograft survival through myeloid cells
Julian K. Horwitz, … , Paolo Cravedi, Peter S. Heeger
Julian K. Horwitz, … , Paolo Cravedi, Peter S. Heeger
Published April 7, 2022
Citation Information: JCI Insight. 2022;7(10):e158856. https://doi.org/10.1172/jci.insight.158856.
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Research Article Transplantation

Linking erythropoietin to Treg-dependent allograft survival through myeloid cells

Abstract

Erythropoietin (EPO) has multiple nonerythropoietic functions, including immune modulation, but EPO’s effects in transplantation remain incompletely understood. We tested the mechanisms linking EPO administration to prolongation of murine heterotopic heart transplantation using WT and conditional EPO receptor–knockout (EPOR-knockout) mice as recipients. In WT controls, peritransplant administration of EPO synergized with CTLA4-Ig to prolong allograft survival (P < 0.001), reduce frequencies of donor-reactive effector CD8+ T cells in the spleen (P < 0.001) and in the graft (P < 0.05), and increase frequencies and total numbers of donor-reactive Tregs (P < 0.01 for each) versus CTLA4-Ig alone. Studies performed in conditional EPOR-knockout recipients showed that each of these differences required EPOR expression in myeloid cells but not in T cells. Analysis of mRNA isolated from spleen monocytes showed that EPO/EPOR ligation upregulated macrophage-expressed, antiinflammatory, regulatory, and pro-efferocytosis genes and downregulated selected proinflammatory genes. Taken together, the data support the conclusion that EPO promotes Treg-dependent murine cardiac allograft survival by crucially altering the phenotype and function of macrophages. Coupled with our previous documentation that EPO promotes Treg expansion in humans, the data support the need for testing the addition of EPO to costimulatory blockade-containing immunosuppression regimens in an effort to prolong human transplant survival.

Authors

Julian K. Horwitz, Sofia Bin, Robert L. Fairchild, Karen S. Keslar, Zhengzi Yi, Weijia Zhang, Vasile I. Pavlov, Yansui Li, Joren C. Madsen, Paolo Cravedi, Peter S. Heeger

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Figure 1

EPO synergizes with CTLA4-Ig to prolong heart transplant survival through ligation of EPOR expressed on myeloid cells.

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EPO synergizes with CTLA4-Ig to prolong heart transplant survival throug...
(A) Schematic of design and treatment regimen. (B) Survival of BALB/c hearts transplanted into WT B6 recipients and either not treated (n = 3) or treated with EPO alone (n = 3), CTLA4-Ig alone (n = 4), or EPO+CTLA4-Ig (n = 5). Results compared among groups by Kaplan-Meier (log-rank) survival analysis. (C) Representative flow cytometry plots of intracellular pSTAT5 in splenic myeloid or nonmyeloid cells obtained from EPORfl/fl or EPORfl/fl LysM-Cre animals 30 minutes after in vitro treatment with vehicle or EPO as indicated. (D) Quantified results (n = 3/group) of pSTAT5 in splenic myeloid cells isolated from EPORfl/fl or EPORfl/fl LysM-Cre animals 30 minutes after in vitro treatment with vehicle or EPO. Statistics in D compared by 2-tailed Student’s t test. Representative of 2 independent experiments. (E) Survival of BALB/c hearts transplanted into B6 EPORfl/fl, EPORfl/fl LysM-Cre, or EPORfl/fl CD4-Cre recipients and treated with or without CTLA4-Ig and with or without EPO as indicated. Results compared among groups by Kaplan-Meier (log-rank) survival analysis. n = 6 per group except for untreated EPORfl/fl and EPORfl/fl LysM-Cre (n = 3/group). *P < 0.05; ***P < 0.001; NS, not significant.