Epigenetic Analysis of the Chromatin Landscape Identifies a Repertoire of Murine Eosinophil-Specific PU.1-Bound Enhancers

Epigenetic Analysis of the Chromatin Landscape Identifies a Repertoire of Murine Eosinophil-Specific PU.1-Bound Enhancers

Eosinophils develop in the bone marrow from hematopoietic progenitors into mature cells capable of a plethora of immunomodulatory roles via the choreographed process of eosinophilopoiesis. However, the gene regulatory elements and transcription factors (TFs) orchestrating this process remain largely...

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Veröffentlicht in:The Journal of immunology (1950) 2021-08, Vol.207 (4), p.1044-1054
Hauptverfasser: Felton, Jennifer M., Vallabh, Sushmitha, Parameswaran, Sreeja, Edsall, Lee E., Ernst, Kevin, Wronowski, Benjamin, Malik, Astha, Kotliar, Michael, Weirauch, Matthew T., Barski, Artem, Fulkerson, Patricia C., Rothenberg, Marc E.
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container_end_page 1054
container_issue 4
container_start_page 1044
container_title The Journal of immunology (1950)
container_volume 207
creator Felton, Jennifer M.
Vallabh, Sushmitha
Parameswaran, Sreeja
Edsall, Lee E.
Ernst, Kevin
Wronowski, Benjamin
Malik, Astha
Kotliar, Michael
Weirauch, Matthew T.
Barski, Artem
Fulkerson, Patricia C.
Rothenberg, Marc E.
description Eosinophils develop in the bone marrow from hematopoietic progenitors into mature cells capable of a plethora of immunomodulatory roles via the choreographed process of eosinophilopoiesis. However, the gene regulatory elements and transcription factors (TFs) orchestrating this process remain largely unknown. The potency and resulting diversity fundamental to an eosinophil's complex immunomodulatory functions and tissue specialization likely result from dynamic epigenetic regulation of the eosinophil genome, a dynamic eosinophil regulome. In this study, we applied a global approach using broad-range, next-generation sequencing to identify a repertoire of eosinophil-specific enhancers. We identified over 8200 active enhancers located within 1-20 kB of expressed eosinophil genes. TF binding motif analysis revealed PU.1 (Spit) motif enrichment in eosinophil enhancers, and chromatin immunoprecipitation coupled with massively parallel sequencing confirmed PU.1 binding in likely enhancers of genes highly expressed in eosinophils. A substantial proportion (>25%) of these PU.1-bound enhancers were unique to murine, culture-derived eosinophils when compared among enhancers of highly expressed genes of three closely related myeloid cell subsets (macrophages, neutrophils, and immature granulocytes). Gene ontology analysis of eosinophil-specific, PU.1bound enhancers revealed enrichment for genes involved in migration, proliferation, degranulation, and survival. Furthermore, eosinophil-specific superenhancers were enriched in genes whose homologs are associated with risk loci for eosinophilia and allergic diseases. Our collective data identify eosinophil-specific enhancers regulating key eosinophil genes through epigenetic mechanisms (H3K27 acetylation) and TF binding (PU.1).
doi_str_mv 10.4049/jimmunol.2000207
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subjects Immunology
Life Sciences & Biomedicine
Science & Technology
title Epigenetic Analysis of the Chromatin Landscape Identifies a Repertoire of Murine Eosinophil-Specific PU.1-Bound Enhancers
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