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Literature DB >> 26797145

Lineage-specific enhancers activate self-renewal genes in macrophages and embryonic stem cells.

Erinn L Soucie¹, Ziming Weng², Laufey Geirsdóttir³, Kaaweh Molawi⁴, Julien Maurizio³, Romain Fenouil³, Noushine Mossadegh-Keller³, Gregory Gimenez³, Laurent VanHille³, Meryam Beniazza³, Jeremy Favret³, Carole Berruyer³, Pierre Perrin³, Nir Hacohen⁵, J-C Andrau⁶, Pierre Ferrier³, Patrice Dubreuil⁷, Arend Sidow⁸, Michael H Sieweke⁹.

Abstract

Differentiated macrophages can self-renew in tissues and expand long term in culture, but the gene regulatory mechanisms that accomplish self-renewal in the differentiated state have remained unknown. Here we show that in mice, the transcription factors MafB and c-Maf repress a macrophage-specific enhancer repertoire associated with a gene network that controls self-renewal. Single-cell analysis revealed that, in vivo, proliferating resident macrophages can access this network by transient down-regulation of Maf transcription factors. The network also controls embryonic stem cell self-renewal but is associated with distinct embryonic stem cell-specific enhancers. This indicates that distinct lineage-specific enhancer platforms regulate a shared network of genes that control self-renewal potential in both stem and mature cells.

Entities: Chemical Disease Gene Mutation Species

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Year: 2016 PMID： 26797145 PMCID： PMC4811353 DOI： 10.1126/science.aad5510

Source DB: PubMed Journal: Science ISSN： 0036-8075 Impact factor: 47.728

39 in total

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Journal: Cell Stem Cell Date: 2009-04-02 Impact factor: 24.633

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Authors: Athar Aziz; Erinn Soucie; Sandrine Sarrazin; Michael H Sieweke
Journal: Science Date: 2009-11-06 Impact factor: 47.728

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Authors: Michael H Sieweke; Judith E Allen
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4. Three Unique Interstitial Macrophages in the Murine Lung at Steady State.

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Review 9. Transcription Factor Bhlhe40 in Immunity and Autoimmunity.

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