Donor T cell DNMT3a regulates alloreactivity in mouse models of hematopoietic stem cell transplantation
Yiouli P. Ktena, … , Christopher J. Gamper, Kenneth R. Cooke
Yiouli P. Ktena, … , Christopher J. Gamper, Kenneth R. Cooke
Published May 24, 2022
Citation Information: J Clin Invest. 2022;132(13):e158047. https://doi.org/10.1172/JCI158047.
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Research Article

Donor T cell DNMT3a regulates alloreactivity in mouse models of hematopoietic stem cell transplantation

Abstract

DNA methyltransferase 3a (DNMT3a) is an important part of the epigenetic machinery that stabilizes patterns of activated T cell responses. We hypothesized that donor T cell DNMT3a regulates alloreactivity after allogeneic blood and marrow transplantation (allo-BMT). T cell conditional Dnmt3a KO mice were used as donors in allo-BMT models. Mice receiving allo-BMT from KO donors developed severe acute graft-versus-host disease (aGVHD), with increases in inflammatory cytokine levels and organ histopathology scores. KO T cells migrated and proliferated in secondary lymphoid organs earlier and demonstrated an advantage in trafficking to the small intestine. Donor T cell subsets were purified after BMT for whole-genome bisulfite sequencing (WGBS) and RNA-Seq. KO T cells had global methylation similar to that of WT cells, with distinct, localized areas of hypomethylation. Using a highly sensitive computational method, we produced a comprehensive profile of the altered epigenome landscape. Hypomethylation corresponded with changes in gene expression in several pathways of T cell signaling and differentiation. Additionally, Dnmt3a-KO T cells resulted in superior graft-versus-tumor activity. Our findings demonstrate a critical role for DNMT3a in regulating T cell alloreactivity and reveal pathways that control T cell tolerance. These results also provide a platform for deciphering clinical data that associate donor DNMT3a mutations with increased GVHD, decreased relapse, and improved survival.

Authors

Yiouli P. Ktena, Michael A. Koldobskiy, Michael I. Barbato, Han-Hsuan Fu, Leo Luznik, Nicolas J. Llosa, Azeb Haile, Orly R. Klein, Chen Liu, Christopher J. Gamper, Kenneth R. Cooke

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Figure 7

Alterations in methylome and transcriptome provide mechanistic clues for enhanced GVHD severity.

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Alterations in methylome and transcriptome provide mechanistic clues for...
(A) Close-up view of the heatmap presented in Figure 6D. (B) CCR9 expression by flow cytometry in the migration experiments presented in Figure 4B. On day +4, most of the CCR9+ cells in the spleen are WT, while the cells that have started migrating toward the MLNs, PPs, IELs, and LP are mostly KO. Data from 2 experiments; n = 8 per group (except MLNs n = 5). (C) MFI of CCR9. (D) PD-1 and TIM3 expression on CD4+ and CD8+ cells on day +7 in the B6→F1 model (top row: percentage of splenic T cells; bottom row: absolute numbers). No differences were detected in LAG3 expression. Data from 2 different experiments; Syn n = 8, Allo n = 9 per group. *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001, Mann-Whitney U test or Mantel-Cox log-rank test for survival data.