The transcription factor NR4A1 is essential for the development of a novel macrophage subset in the thymus

Robert Tacke; Ingo Hilgendorf; Hannah Garner; Claire Waterborg; Kiwon Park; Heba Nowyhed; Richard N Hanna; Runpei Wu; Filip K Swirski; Frederic Geissmann; Catherine C Hedrick

doi:10.1038/srep10055

The transcription factor NR4A1 is essential for the development of a novel macrophage subset in the thymus

Robert Tacke, Ingo Hilgendorf, Hannah Garner, Claire Waterborg, Kiwon Park, Heba Nowyhed, Richard N Hanna, Runpei Wu, Filip K Swirski, Frederic Geissmann, Catherine C Hedrick

Inflammation Biology

Research output: Contribution to journal › Article › peer-review

42 Citations (Scopus)

Abstract

Tissue macrophages function to maintain homeostasis and regulate immune responses. While tissue macrophages derive from one of a small number of progenitor programs, the transcriptional requirements for site-specific macrophage subset development are more complex. We have identified a new tissue macrophage subset in the thymus and have discovered that its development is dependent on transcription factor NR4A1. Functionally, we find that NR4A1-dependent macrophages are critically important for clearance of apoptotic thymocytes. These macrophages are largely reduced or absent in mice lacking NR4A1, and Nr4a1-deficient mice have impaired thymocyte engulfment and clearance. Thus, NR4A1 functions as a master transcription factor for the development of this novel thymus-specific macrophage subset.

Original language	English
Article number	10055
Number of pages	13
Journal	Scientific Reports
Volume	5
DOIs	https://doi.org/10.1038/srep10055
Publication status	Published - 19 Jun 2015

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title = "The transcription factor NR4A1 is essential for the development of a novel macrophage subset in the thymus",

abstract = "Tissue macrophages function to maintain homeostasis and regulate immune responses. While tissue macrophages derive from one of a small number of progenitor programs, the transcriptional requirements for site-specific macrophage subset development are more complex. We have identified a new tissue macrophage subset in the thymus and have discovered that its development is dependent on transcription factor NR4A1. Functionally, we find that NR4A1-dependent macrophages are critically important for clearance of apoptotic thymocytes. These macrophages are largely reduced or absent in mice lacking NR4A1, and Nr4a1-deficient mice have impaired thymocyte engulfment and clearance. Thus, NR4A1 functions as a master transcription factor for the development of this novel thymus-specific macrophage subset.",

author = "Robert Tacke and Ingo Hilgendorf and Hannah Garner and Claire Waterborg and Kiwon Park and Heba Nowyhed and Hanna, {Richard N} and Runpei Wu and Swirski, {Filip K} and Frederic Geissmann and Hedrick, {Catherine C}",

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T1 - The transcription factor NR4A1 is essential for the development of a novel macrophage subset in the thymus

AU - Tacke, Robert

AU - Hilgendorf, Ingo

AU - Garner, Hannah

AU - Waterborg, Claire

AU - Park, Kiwon

AU - Nowyhed, Heba

AU - Hanna, Richard N

AU - Wu, Runpei

AU - Swirski, Filip K

AU - Geissmann, Frederic

AU - Hedrick, Catherine C

PY - 2015/6/19

Y1 - 2015/6/19

N2 - Tissue macrophages function to maintain homeostasis and regulate immune responses. While tissue macrophages derive from one of a small number of progenitor programs, the transcriptional requirements for site-specific macrophage subset development are more complex. We have identified a new tissue macrophage subset in the thymus and have discovered that its development is dependent on transcription factor NR4A1. Functionally, we find that NR4A1-dependent macrophages are critically important for clearance of apoptotic thymocytes. These macrophages are largely reduced or absent in mice lacking NR4A1, and Nr4a1-deficient mice have impaired thymocyte engulfment and clearance. Thus, NR4A1 functions as a master transcription factor for the development of this novel thymus-specific macrophage subset.

AB - Tissue macrophages function to maintain homeostasis and regulate immune responses. While tissue macrophages derive from one of a small number of progenitor programs, the transcriptional requirements for site-specific macrophage subset development are more complex. We have identified a new tissue macrophage subset in the thymus and have discovered that its development is dependent on transcription factor NR4A1. Functionally, we find that NR4A1-dependent macrophages are critically important for clearance of apoptotic thymocytes. These macrophages are largely reduced or absent in mice lacking NR4A1, and Nr4a1-deficient mice have impaired thymocyte engulfment and clearance. Thus, NR4A1 functions as a master transcription factor for the development of this novel thymus-specific macrophage subset.

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DO - 10.1038/srep10055

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C2 - 26091486

SN - 2045-2322

VL - 5

JO - Scientific Reports

JF - Scientific Reports

M1 - 10055

ER -

The transcription factor NR4A1 is essential for the development of a novel macrophage subset in the thymus

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