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Schistosomiasis Induces Persistent DNA Methylation and Tuberculosis-Specific Immune Changes
Andrew R. DiNardo, Tomoki Nishiguchi, Emily M. Mace, Kimal Rajapakshe, Godwin Mtetwa, Alexander Kay, Gugu Maphalala, W. Evan Secor, Rojelio Mejía, Jordan S. Orange, Cristian Coarfa, Kapil N. Bhalla, Edward A. Graviss, Anna M. Mandalakas, George Makedonas
The Journal of Immunology · 2018 · ▲ 72 citations
Abstract
Abstract Epigenetic mechanisms, such as DNA methylation, determine immune cell phenotype. To understand the epigenetic alterations induced by helminth coinfections, we evaluated the longitudinal effect of ascariasis and schistosomiasis infection on CD4+ T cell DNA methylation and the downstream tuberculosis (TB)–specific and bacillus Calmette–Guérin–induced immune phenotype. All experiments were performed on human primary immune cells from a longitudinal cohort of recently TB-exposed children. Compared with age-matched uninfected controls, children with active Schistosoma haematobium and Ascaris lumbricoides infection had 751 differentially DNA-methylated genes, with 72% hypermethylated. Gene ontology pathway analysis identified inhibition of IFN-γ signaling, cellular proliferation, and the Th1 pathway. Targeted real-time quantitative PCR after methyl-specific endonuclease digestion confirmed DNA hypermethylation of the transcription factors BATF3, ID2, STAT5A, IRF5, PPARg, RUNX2, IRF4, and NFATC1 and cytokines or cytokine receptors IFNGR1, TNFS11, RELT (TNF receptor), IL12RB2, and IL12B (p < 0.001; Sidak–Bonferroni). Functional blockage of the IFN-γ signaling pathway was confirmed, with helminth-infected individuals having decreased upregulation of IFN-γ–inducible genes (Mann–Whitney p < 0.05). Hypomethylation of the IL-4 pathway and DNA hypermethylation of the Th1 pathway was confirmed by Ag-specific multidimensional flow cytometry demonstrating decreased TB-specific IFN-γ and TNF and increased IL-4 production by CD4+ T cells (Wilcoxon signed-rank p < 0.05). In S. haematobium–infected individuals, these DNA methylation and immune phenotypic changes persisted at least 6 mo after successful deworming. This work demonstrates that helminth infection induces DNA methylation and immune perturbations that inhibit TB-specific immune control and that the duration of these changes are helminth specific.
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- 10.4049/jimmunol.1800101
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- 2026-06-03 MST
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APA
DiNardo, A.R., Nishiguchi, T., Mace, E.M., Rajapakshe, K., Mtetwa, G., Kay, A., Maphalala, G., Secor, W.E., Mejía, R., Orange, J.S., Coarfa, C., Bhalla, K.N., Graviss, E.A., Mandalakas, A.M., & Makedonas, G. (2018). Schistosomiasis Induces Persistent DNA Methylation and Tuberculosis-Specific Immune Changes. <em>The Journal of Immunology</em>. https://doi.org/10.4049/jimmunol.1800101
Vancouver
DiNardo AR, Nishiguchi T, Mace EM, Rajapakshe K, Mtetwa G, Kay A, et al. Schistosomiasis Induces Persistent DNA Methylation and Tuberculosis-Specific Immune Changes. The Journal of Immunology. 2018. doi:10.4049/jimmunol.1800101.
BibTeX
@article{andrew2018Schist,
title = {Schistosomiasis Induces Persistent DNA Methylation and Tuberculosis-Specific Immune Changes},
author = {Andrew R. DiNardo and Tomoki Nishiguchi and Emily M. Mace and Kimal Rajapakshe and Godwin Mtetwa and Alexander Kay and Gugu Maphalala and W. Evan Secor and Rojelio Mejía and Jordan S. Orange and Cristian Coarfa and Kapil N. Bhalla and Edward A. Graviss and Anna M. Mandalakas and George Makedonas},
journal = {The Journal of Immunology},
year = {2018},
doi = {10.4049/jimmunol.1800101},
}
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