Bhlhe40 and Bhlhe41 transcription factors regulate alveolar macrophage self-renewal and identity.
René Rauschmeier,Charlotte Gustafsson,Annika Reinhardt,Annika Reinhardt,Noelia A-Gonzalez,Luigi Tortola,Dilay Cansever,Sethuraman Subramanian,Sethuraman Subramanian,Reshma Taneja,Moritz J. Rossner,Michael H. Sieweke,Michael H. Sieweke,Melanie Greter,Robert Månsson,Robert Månsson,Meinrad Busslinger,Taras Kreslavsky,Taras Kreslavsky,Taras Kreslavsky +19 more
TL;DR: In this article, the authors identify the transcription factors Bhlhe40/Bhlhe41 as novel regulators of alveolar macrophages (AMs), a population that provides the first line of immune defense and executes homeostatic functions.
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Abstract: Tissues in multicellular organisms are populated by resident macrophages, which perform both generic and tissue-specific functions. The latter are induced by signals from the microenvironment and rely on unique tissue-specific molecular programs requiring the combinatorial action of tissue-specific and broadly expressed transcriptional regulators. Here, we identify the transcription factors Bhlhe40 and Bhlhe41 as novel regulators of alveolar macrophages (AMs)-a population that provides the first line of immune defense and executes homeostatic functions in lung alveoli. In the absence of these factors, AMs exhibited decreased proliferation that resulted in a severe disadvantage of knockout AMs in a competitive setting. Gene expression analyses revealed a broad cell-intrinsic footprint of Bhlhe40/Bhlhe41 deficiency manifested by a downregulation of AM signature genes and induction of signature genes of other macrophage lineages. Genome-wide characterization of Bhlhe40 DNA binding suggested that these transcription factors directly repress the expression of lineage-inappropriate genes in AMs. Taken together, these results identify Bhlhe40 and Bhlhe41 as key regulators of AM self-renewal and guardians of their identity.
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