DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas

Laura Herrtwich; Indrajit Nanda; Konstantinos Evangelou; Teodora Nikolova; Veronika Horn; null Sagar; Daniel Erny; Jonathan Stefanowski; Leif Rogell; Claudius Klein; Kourosh Gharun; Marie Follo; Maximilian Seidl; Bernhard Kremer; Nikolas Muenke; Julia Senges; Manfred Fliegauf; Tom Aschman; Dietmar Pfeifer; Sandrine Sarrazin; Michael H. Sieweke; Dirk Wagner; Christine Dierks; Thomas Haaf; Thomas Ness; Mario M. Zaiss; Reinhard E. Voll; Sachin D. Deshmukh; Marco Prinz; Torsten Goldmann; Christoph Hoelscher; Anja E. Hauser; Andres J. Lopez-Contreras; Dominic Gruen; Vassilis Gorgoulis; Andreas Diefenbach; Philipp Henneke; Antigoni Triantafyllopoulou

doi:10.1016/j.cell.2016.09.054

DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas

Laura Herrtwich, Indrajit Nanda, Konstantinos Evangelou, Teodora Nikolova, Veronika Horn, Sagar, Daniel Erny, Jonathan Stefanowski, Leif Rogell, Claudius Klein, Kourosh Gharun, Marie Follo, Maximilian Seidl, Bernhard Kremer, Nikolas Muenke, Julia Senges, Manfred Fliegauf, Tom Aschman, Dietmar Pfeifer, Sandrine SarrazinMichael H. Sieweke, Dirk Wagner, Christine Dierks, Thomas Haaf, Thomas Ness, Mario M. Zaiss, Reinhard E. Voll, Sachin D. Deshmukh, Marco Prinz, Torsten Goldmann, Christoph Hoelscher, Anja E. Hauser, Andres J. Lopez-Contreras, Dominic Gruen, Vassilis Gorgoulis, Andreas Diefenbach, Philipp Henneke, Antigoni Triantafyllopoulou

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

97 Citationer (Scopus)

Abstract

Granulomas are immune cell aggregates formed in response to persistent inflammatory stimuli. Granuloma macrophage subsets are diverse and carry varying copy numbers of their genomic information. The molecular programs that control the differentiation of such macrophage populations in response to a chronic stimulus, though critical for disease outcome, have not been defined. Here, we delineate a macrophage differentiation pathway by which a persistent Toll-like receptor (TLR) 2 signal instructs polyploid macrophage fate by inducing replication stress and activating the DNA damage response. Polyploid granuloma-resident macrophages formed via modified cell divisions and mitotic defects and not, as previously thought, by cell-to-cell fusion. TLR2 signaling promoted macrophage polyploidy and suppressed genomic instability by regulating Myc and ATR. We propose that, in the presence of persistent inflammatory stimuli, pathways previously linked to oncogene-initiated carcinogenesis instruct a long-lived granuloma-resident macrophage differentiation program that regulates granulomatous tissue remodeling.

Originalsprog	Engelsk
Tidsskrift	Cell
Vol/bind	167
Udgave nummer	5
Sider (fra-til)	1264–1280.e18
ISSN	0092-8674
DOI	https://doi.org/10.1016/j.cell.2016.09.054
Status	Udgivet - 17 nov. 2016

Adgang til dokumentet

10.1016/j.cell.2016.09.054

Citationsformater

Herrtwich, L., Nanda, I., Evangelou, K., Nikolova, T., Horn, V., Sagar, Erny, D., Stefanowski, J., Rogell, L., Klein, C., Gharun, K., Follo, M., Seidl, M., Kremer, B., Muenke, N., Senges, J., Fliegauf, M., Aschman, T., Pfeifer, D., ... Triantafyllopoulou, A. (2016). DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas. Cell, 167(5), 1264–1280.e18. https://doi.org/10.1016/j.cell.2016.09.054

Herrtwich, L, Nanda, I, Evangelou, K, Nikolova, T, Horn, V, Sagar, Erny, D, Stefanowski, J, Rogell, L, Klein, C, Gharun, K, Follo, M, Seidl, M, Kremer, B, Muenke, N, Senges, J, Fliegauf, M, Aschman, T, Pfeifer, D, Sarrazin, S, Sieweke, MH, Wagner, D, Dierks, C, Haaf, T, Ness, T, Zaiss, MM, Voll, RE, Deshmukh, SD, Prinz, M, Goldmann, T, Hoelscher, C, Hauser, AE, Lopez-Contreras, AJ, Gruen, D, Gorgoulis, V, Diefenbach, A, Henneke, P & Triantafyllopoulou, A 2016, 'DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas', Cell, bind 167, nr. 5, s. 1264–1280.e18. https://doi.org/10.1016/j.cell.2016.09.054

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title = "DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas",

abstract = "Granulomas are immune cell aggregates formed in response to persistent inflammatory stimuli. Granuloma macrophage subsets are diverse and carry varying copy numbers of their genomic information. The molecular programs that control the differentiation of such macrophage populations in response to a chronic stimulus, though critical for disease outcome, have not been defined. Here, we delineate a macrophage differentiation pathway by which a persistent Toll-like receptor (TLR) 2 signal instructs polyploid macrophage fate by inducing replication stress and activating the DNA damage response. Polyploid granuloma-resident macrophages formed via modified cell divisions and mitotic defects and not, as previously thought, by cell-to-cell fusion. TLR2 signaling promoted macrophage polyploidy and suppressed genomic instability by regulating Myc and ATR. We propose that, in the presence of persistent inflammatory stimuli, pathways previously linked to oncogene-initiated carcinogenesis instruct a long-lived granuloma-resident macrophage differentiation program that regulates granulomatous tissue remodeling.",

author = "Laura Herrtwich and Indrajit Nanda and Konstantinos Evangelou and Teodora Nikolova and Veronika Horn and Sagar and Daniel Erny and Jonathan Stefanowski and Leif Rogell and Claudius Klein and Kourosh Gharun and Marie Follo and Maximilian Seidl and Bernhard Kremer and Nikolas Muenke and Julia Senges and Manfred Fliegauf and Tom Aschman and Dietmar Pfeifer and Sandrine Sarrazin and Sieweke, {Michael H.} and Dirk Wagner and Christine Dierks and Thomas Haaf and Thomas Ness and Zaiss, {Mario M.} and Voll, {Reinhard E.} and Deshmukh, {Sachin D.} and Marco Prinz and Torsten Goldmann and Christoph Hoelscher and Hauser, {Anja E.} and Lopez-Contreras, {Andres J.} and Dominic Gruen and Vassilis Gorgoulis and Andreas Diefenbach and Philipp Henneke and Antigoni Triantafyllopoulou",

year = "2016",

month = nov,

day = "17",

doi = "10.1016/j.cell.2016.09.054",

language = "English",

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journal = "Cell",

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T1 - DNA Damage Signaling Instructs Polyploid Macrophage Fate in Granulomas

AU - Herrtwich, Laura

AU - Nanda, Indrajit

AU - Evangelou, Konstantinos

AU - Nikolova, Teodora

AU - Horn, Veronika

AU - Sagar, null

AU - Erny, Daniel

AU - Stefanowski, Jonathan

AU - Rogell, Leif

AU - Klein, Claudius

AU - Gharun, Kourosh

AU - Follo, Marie

AU - Seidl, Maximilian

AU - Kremer, Bernhard

AU - Muenke, Nikolas

AU - Senges, Julia

AU - Fliegauf, Manfred

AU - Aschman, Tom

AU - Pfeifer, Dietmar

AU - Sarrazin, Sandrine

AU - Sieweke, Michael H.

AU - Wagner, Dirk

AU - Dierks, Christine

AU - Haaf, Thomas

AU - Ness, Thomas

AU - Zaiss, Mario M.

AU - Voll, Reinhard E.

AU - Deshmukh, Sachin D.

AU - Prinz, Marco

AU - Goldmann, Torsten

AU - Hoelscher, Christoph

AU - Hauser, Anja E.

AU - Lopez-Contreras, Andres J.

AU - Gruen, Dominic

AU - Gorgoulis, Vassilis

AU - Diefenbach, Andreas

AU - Henneke, Philipp

AU - Triantafyllopoulou, Antigoni

PY - 2016/11/17

Y1 - 2016/11/17

N2 - Granulomas are immune cell aggregates formed in response to persistent inflammatory stimuli. Granuloma macrophage subsets are diverse and carry varying copy numbers of their genomic information. The molecular programs that control the differentiation of such macrophage populations in response to a chronic stimulus, though critical for disease outcome, have not been defined. Here, we delineate a macrophage differentiation pathway by which a persistent Toll-like receptor (TLR) 2 signal instructs polyploid macrophage fate by inducing replication stress and activating the DNA damage response. Polyploid granuloma-resident macrophages formed via modified cell divisions and mitotic defects and not, as previously thought, by cell-to-cell fusion. TLR2 signaling promoted macrophage polyploidy and suppressed genomic instability by regulating Myc and ATR. We propose that, in the presence of persistent inflammatory stimuli, pathways previously linked to oncogene-initiated carcinogenesis instruct a long-lived granuloma-resident macrophage differentiation program that regulates granulomatous tissue remodeling.

AB - Granulomas are immune cell aggregates formed in response to persistent inflammatory stimuli. Granuloma macrophage subsets are diverse and carry varying copy numbers of their genomic information. The molecular programs that control the differentiation of such macrophage populations in response to a chronic stimulus, though critical for disease outcome, have not been defined. Here, we delineate a macrophage differentiation pathway by which a persistent Toll-like receptor (TLR) 2 signal instructs polyploid macrophage fate by inducing replication stress and activating the DNA damage response. Polyploid granuloma-resident macrophages formed via modified cell divisions and mitotic defects and not, as previously thought, by cell-to-cell fusion. TLR2 signaling promoted macrophage polyploidy and suppressed genomic instability by regulating Myc and ATR. We propose that, in the presence of persistent inflammatory stimuli, pathways previously linked to oncogene-initiated carcinogenesis instruct a long-lived granuloma-resident macrophage differentiation program that regulates granulomatous tissue remodeling.

U2 - 10.1016/j.cell.2016.09.054

DO - 10.1016/j.cell.2016.09.054

M3 - Journal article

C2 - 28084216

SN - 0092-8674

VL - 167

SP - 1264–1280.e18

JO - Cell

JF - Cell

IS - 5

ER -