Blockade of individual Notch ligands and receptors controls graft-versus-host disease
Ivy T. Tran, … , Christian W. Siebel, Ivan Maillard
Ivy T. Tran, … , Christian W. Siebel, Ivan Maillard
Published March 1, 2013
Citation Information: J Clin Invest. 2013;123(4):1590-1604. https://doi.org/10.1172/JCI65477.
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Research Article Immunology

Blockade of individual Notch ligands and receptors controls graft-versus-host disease

Abstract

Graft-versus-host disease (GVHD) is the main complication of allogeneic bone marrow transplantation. Current strategies to control GVHD rely on global immunosuppression. These strategies are incompletely effective and decrease the anticancer activity of the allogeneic graft. We previously identified Notch signaling in T cells as a new therapeutic target for preventing GVHD. Notch-deprived T cells showed markedly decreased production of inflammatory cytokines, but normal in vivo proliferation, increased accumulation of regulatory T cells, and preserved anticancer effects. Here, we report that γ-secretase inhibitors can block all Notch signals in alloreactive T cells, but lead to severe on-target intestinal toxicity. Using newly developed humanized antibodies and conditional genetic models, we demonstrate that Notch1/Notch2 receptors and the Notch ligands Delta-like1/4 mediate all the effects of Notch signaling in T cells during GVHD, with dominant roles for Notch1 and Delta-like4. Notch1 inhibition controlled GVHD, but led to treatment-limiting toxicity. In contrast, Delta-like1/4 inhibition blocked GVHD without limiting adverse effects while preserving substantial anticancer activity. Transient blockade in the peritransplant period provided durable protection. These findings open new perspectives for selective and safe targeting of individual Notch pathway components in GVHD and other T cell–mediated human disorders.

Authors

Ivy T. Tran, Ashley R. Sandy, Alexis J. Carulli, Christen Ebens, Jooho Chung, Gloria T. Shan, Vedran Radojcic, Ann Friedman, Thomas Gridley, Amy Shelton, Pavan Reddy, Linda C. Samuelson, Minhong Yan, Christian W. Siebel, Ivan Maillard

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Figure 7

Preserved in vivo T cell proliferation and increased expansion of Tregs upon transient Dll1/Dll4 blockade.

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Preserved in vivo T cell proliferation and increased expansion of Tregs ...
Irradiated BALB/c mice (9 Gy) were infused with TCD BM, with or without WT or DNMAML spleen T cells. Isotype control or anti-Dll1/DllL4 antibodies were administered transiently (days 0, 3, 7, and 10). (A) Preserved in vivo proliferation as assessed by tracking CFSE-labeled donor-derived T cells and (B) BrdU incorporation on day 5 after allo-BMT. (C) Expansion of WT, DNMAML, and WT T cells in anti-Dll1/Dll4–treated mice at days 14, 21, and 35 after transplantation. Graphs show the absolute number of donor-derived H2Kb+H2Kd CD4+ or CD8+ T cells in the spleen of individual recipients. (D) Short-term Dll1/Dll4 inhibition was associated with persistently elevated percentages and absolute number of Tregs at day 35. Representative flow cytometry plots for intracellular FoxP3 staining are shown, including a sample stained with isotype control antibodies. Numbers indicate the percentage of cells in each quadrant. Bar graphs represent mean ± SD. **P < 0.01; *P < 0.05.