A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis

Mourad Matmati; Peggy Jacques; Jonathan Maelfait; Eveline Verheugen; Mirjam Kool; Mozes Sze; Lies Geboes; Els Louagie; Conor Mc Guire; Lars Vereecke; Yuanyuan Chu; Louis Boon; Steven Staelens; Patrick Matthys; Bart N. Lambrecht; Marc Schmidt-Supprian; Manolis Pasparakis; Dirk Elewaut; Rudi Beyaert; Geert Van Loo

doi:10.1038/ng.874

A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis

Mourad Matmati
, Peggy Jacques
, Jonathan Maelfait
, Eveline Verheugen
, Mirjam Kool
, Mozes Sze
, Lies Geboes
, Els Louagie
, Conor Mc Guire
, Lars Vereecke
, Yuanyuan Chu
, Louis Boon
, Steven Staelens
, Patrick Matthys
, Bart N. Lambrecht
, Marc Schmidt-Supprian
, Manolis Pasparakis
, Dirk Elewaut
, Rudi Beyaert
, Geert Van Loo

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

257 Scopus citations

Abstract

A20 (TNFAIP3) is a protein that is involved in the negative feedback regulation of NF-°B signaling in response to specific proinflammatory stimuli in different cell types and has been suggested as a susceptibility gene for rheumatoid arthritis. To define the contribution of A20 to rheumatoid arthritis pathology, we generated myeloid-specific A20-deficient mice and show that specific ablation of Tnfaip3 in myeloid cells results in spontaneous development of a severe destructive polyarthritis with many features of rheumatoid arthritis. Myeloid-A20-deficient mice have high levels of inflammatory cytokines in their serum, consistent with a sustained NF-°B activation and higher TNF production by macrophages. Destructive polyarthritis in myeloid A20 knockout mice was TLR4-MyD88 and IL-6 dependent but was TNF independent. Myeloid A20 deficiency also promoted osteoclastogenesis in mice. Together, these observations indicate a critical and cell-specific function for A20 in the etiology of rheumatoid arthritis, supporting the idea of developing A20 modulatory drugs as cell-targeted therapies.

Original language	English
Pages (from-to)	908-912
Number of pages	5
Journal	Nature Genetics
Volume	43
Issue number	9
DOIs	https://doi.org/10.1038/ng.874
State	Published - Sep 2011
Externally published	Yes

Access to Document

10.1038/ng.874

Cite this

Matmati, M., Jacques, P., Maelfait, J., Verheugen, E., Kool, M., Sze, M., Geboes, L., Louagie, E., Guire, C. M., Vereecke, L., Chu, Y., Boon, L., Staelens, S., Matthys, P., Lambrecht, B. N., Schmidt-Supprian, M., Pasparakis, M., Elewaut, D., Beyaert, R., & Van Loo, G. (2011). A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis. Nature Genetics, 43(9), 908-912. https://doi.org/10.1038/ng.874

@article{3bd795f0e20e4adf802d1fe625d704ba,

title = "A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis",

abstract = "A20 (TNFAIP3) is a protein that is involved in the negative feedback regulation of NF-°B signaling in response to specific proinflammatory stimuli in different cell types and has been suggested as a susceptibility gene for rheumatoid arthritis. To define the contribution of A20 to rheumatoid arthritis pathology, we generated myeloid-specific A20-deficient mice and show that specific ablation of Tnfaip3 in myeloid cells results in spontaneous development of a severe destructive polyarthritis with many features of rheumatoid arthritis. Myeloid-A20-deficient mice have high levels of inflammatory cytokines in their serum, consistent with a sustained NF-°B activation and higher TNF production by macrophages. Destructive polyarthritis in myeloid A20 knockout mice was TLR4-MyD88 and IL-6 dependent but was TNF independent. Myeloid A20 deficiency also promoted osteoclastogenesis in mice. Together, these observations indicate a critical and cell-specific function for A20 in the etiology of rheumatoid arthritis, supporting the idea of developing A20 modulatory drugs as cell-targeted therapies.",

author = "Mourad Matmati and Peggy Jacques and Jonathan Maelfait and Eveline Verheugen and Mirjam Kool and Mozes Sze and Lies Geboes and Els Louagie and Guire, \{Conor Mc\} and Lars Vereecke and Yuanyuan Chu and Louis Boon and Steven Staelens and Patrick Matthys and Lambrecht, \{Bart N.\} and Marc Schmidt-Supprian and Manolis Pasparakis and Dirk Elewaut and Rudi Beyaert and \{Van Loo\}, Geert",

note = "Funding Information: We are grateful to I. F{\"o}rster for donating the LysM-Cre transgenic mice. We thank H. Heremans for providing us with the IL-6 and control antibodies. We thank T. Hochepied for transgenic services, P. Bogaert and E. Parthoens for technical help, A. Bredan for critical reading of the manuscript and D. Huyghebaert and L. Bellen for animal care. L.V. and J.M. are PhD fellows with the Instituut voor Innovatie door Wetenschap en Technologie (IWT), and J.M. is also supported by an Emmanuel van der Schueren award. C.M.G., L.G. and P.J. are PhD fellows with the Fonds voor Wetenschappelijk Onderzoek-Vlaanderen (FWO). G.v.L. is supported, as a postdoctoral researcher, by the FWO, by an FWO Odysseus Grant and by the Charcot Foundation. M.K. is supported by an Intra European fellowship from the Marie Curie Actions. M.P. is supported by an FP7 EC program grant Masterswitch (EC-223404). B.N.L. is supported by an FWO Odysseus grant, a European Research Council Starting grant and the Group-ID Multidisciplinary Research Partnership grant of Ghent University. Work in the lab of R.B. and G.v.L. is further supported by research grants from the Interuniversity Attraction Poles program (IAP6/18), the FWO, the Belgian Foundation against Cancer, the Strategic Basis Research program of the IWT, the Centrum voor Gezwelziekten, the Hercules Foundation, and the Concerted Research Actions (GOA) and Group-ID MRP of Ghent University.",

year = "2011",

month = sep,

doi = "10.1038/ng.874",

language = "English",

volume = "43",

pages = "908--912",

journal = "Nature Genetics",

issn = "1061-4036",

publisher = "Nature Research",

number = "9",

}

Matmati, M, Jacques, P, Maelfait, J, Verheugen, E, Kool, M, Sze, M, Geboes, L, Louagie, E, Guire, CM, Vereecke, L, Chu, Y, Boon, L, Staelens, S, Matthys, P, Lambrecht, BN, Schmidt-Supprian, M, Pasparakis, M, Elewaut, D, Beyaert, R & Van Loo, G 2011, 'A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis', Nature Genetics, vol. 43, no. 9, pp. 908-912. https://doi.org/10.1038/ng.874

TY - JOUR

T1 - A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis

AU - Matmati, Mourad

AU - Jacques, Peggy

AU - Maelfait, Jonathan

AU - Verheugen, Eveline

AU - Kool, Mirjam

AU - Sze, Mozes

AU - Geboes, Lies

AU - Louagie, Els

AU - Guire, Conor Mc

AU - Vereecke, Lars

AU - Chu, Yuanyuan

AU - Boon, Louis

AU - Staelens, Steven

AU - Matthys, Patrick

AU - Lambrecht, Bart N.

AU - Schmidt-Supprian, Marc

AU - Pasparakis, Manolis

AU - Elewaut, Dirk

AU - Beyaert, Rudi

AU - Van Loo, Geert

N1 - Funding Information: We are grateful to I. Förster for donating the LysM-Cre transgenic mice. We thank H. Heremans for providing us with the IL-6 and control antibodies. We thank T. Hochepied for transgenic services, P. Bogaert and E. Parthoens for technical help, A. Bredan for critical reading of the manuscript and D. Huyghebaert and L. Bellen for animal care. L.V. and J.M. are PhD fellows with the Instituut voor Innovatie door Wetenschap en Technologie (IWT), and J.M. is also supported by an Emmanuel van der Schueren award. C.M.G., L.G. and P.J. are PhD fellows with the Fonds voor Wetenschappelijk Onderzoek-Vlaanderen (FWO). G.v.L. is supported, as a postdoctoral researcher, by the FWO, by an FWO Odysseus Grant and by the Charcot Foundation. M.K. is supported by an Intra European fellowship from the Marie Curie Actions. M.P. is supported by an FP7 EC program grant Masterswitch (EC-223404). B.N.L. is supported by an FWO Odysseus grant, a European Research Council Starting grant and the Group-ID Multidisciplinary Research Partnership grant of Ghent University. Work in the lab of R.B. and G.v.L. is further supported by research grants from the Interuniversity Attraction Poles program (IAP6/18), the FWO, the Belgian Foundation against Cancer, the Strategic Basis Research program of the IWT, the Centrum voor Gezwelziekten, the Hercules Foundation, and the Concerted Research Actions (GOA) and Group-ID MRP of Ghent University.

PY - 2011/9

Y1 - 2011/9

N2 - A20 (TNFAIP3) is a protein that is involved in the negative feedback regulation of NF-°B signaling in response to specific proinflammatory stimuli in different cell types and has been suggested as a susceptibility gene for rheumatoid arthritis. To define the contribution of A20 to rheumatoid arthritis pathology, we generated myeloid-specific A20-deficient mice and show that specific ablation of Tnfaip3 in myeloid cells results in spontaneous development of a severe destructive polyarthritis with many features of rheumatoid arthritis. Myeloid-A20-deficient mice have high levels of inflammatory cytokines in their serum, consistent with a sustained NF-°B activation and higher TNF production by macrophages. Destructive polyarthritis in myeloid A20 knockout mice was TLR4-MyD88 and IL-6 dependent but was TNF independent. Myeloid A20 deficiency also promoted osteoclastogenesis in mice. Together, these observations indicate a critical and cell-specific function for A20 in the etiology of rheumatoid arthritis, supporting the idea of developing A20 modulatory drugs as cell-targeted therapies.

AB - A20 (TNFAIP3) is a protein that is involved in the negative feedback regulation of NF-°B signaling in response to specific proinflammatory stimuli in different cell types and has been suggested as a susceptibility gene for rheumatoid arthritis. To define the contribution of A20 to rheumatoid arthritis pathology, we generated myeloid-specific A20-deficient mice and show that specific ablation of Tnfaip3 in myeloid cells results in spontaneous development of a severe destructive polyarthritis with many features of rheumatoid arthritis. Myeloid-A20-deficient mice have high levels of inflammatory cytokines in their serum, consistent with a sustained NF-°B activation and higher TNF production by macrophages. Destructive polyarthritis in myeloid A20 knockout mice was TLR4-MyD88 and IL-6 dependent but was TNF independent. Myeloid A20 deficiency also promoted osteoclastogenesis in mice. Together, these observations indicate a critical and cell-specific function for A20 in the etiology of rheumatoid arthritis, supporting the idea of developing A20 modulatory drugs as cell-targeted therapies.

UR - https://www.scopus.com/pages/publications/80052195163

U2 - 10.1038/ng.874

DO - 10.1038/ng.874

M3 - Article

C2 - 21841782

AN - SCOPUS:80052195163

SN - 1061-4036

VL - 43

SP - 908

EP - 912

JO - Nature Genetics

JF - Nature Genetics

IS - 9

ER -

A20 (TNFAIP3) deficiency in myeloid cells triggers erosive polyarthritis resembling rheumatoid arthritis

Abstract

Access to Document

Other files and links

Fingerprint

Cite this