Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis

Audrey Paoletti; Bineta Ly; Samuel Bitoun; Gaëtane Nocturne; Elodie Rivière; Jessica J. Manson; Andrea Matucci; Marc Pallardy; Niek de Vries; Xavier Mariette

doi:10.3389/fimmu.2022.832117

Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis

Audrey Paoletti^*, Bineta Ly, Samuel Bitoun, Gaëtane Nocturne, Elodie Rivière, Jessica J. Manson, Andrea Matucci, Marc Pallardy, Niek de Vries, Xavier Mariette

^*Corresponding author for this work

AII - Inflammatory diseases

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

Abstract

Introduction: We previously reported a specific defect of rheumatoid arthritis (RA) monocyte polarization to anti-inflammatory M2-like macrophages related to increased miR-155 expression in all RA patients except those receiving adalimumab (ADA). In this longitudinal study, we examined whether different tumor necrosis factor inhibitors were able to restore monocyte polarization to M2-like macrophages and their effect on the transcriptomic signature. Methods: M2-like polarization induced by human serum AB was studied in 7 healthy donors and 20 RA patients included in the ABIRA cohort before and 3 months after starting ADA or etanercept (ETA). The differential gene expression of M2- and M1-related transcripts was studied in macrophage-derived monocytes after differentiation. Results: At baseline, RA monocytes showed a defect of polarization to M2-like macrophages as compared with healthy donor monocytes, which was negatively correlated with disease activity. M2-like polarization from circulating monocytes was restored only with ADA and not ETA treatment. The transcriptomic signature demonstrated downregulation of M2-related transcripts and upregulation of M1-related transcripts in active RA. In patients receiving ADA, the transcriptomic signature of M2-related transcripts was restored. Conclusion: This longitudinal study demonstrates that ADA but not ETA is able to restore the M2-like polarization of monocytes that is defective in RA.

Original language	English
Article number	832117
Journal	Frontiers in Immunology
Volume	13
DOIs	https://doi.org/10.3389/fimmu.2022.832117
Publication status	Published - 23 Feb 2022

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10.3389/fimmu.2022.832117

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@article{b7ee103eb6bd4958a24183fb61861210,

title = "Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis",

abstract = "Introduction: We previously reported a specific defect of rheumatoid arthritis (RA) monocyte polarization to anti-inflammatory M2-like macrophages related to increased miR-155 expression in all RA patients except those receiving adalimumab (ADA). In this longitudinal study, we examined whether different tumor necrosis factor inhibitors were able to restore monocyte polarization to M2-like macrophages and their effect on the transcriptomic signature. Methods: M2-like polarization induced by human serum AB was studied in 7 healthy donors and 20 RA patients included in the ABIRA cohort before and 3 months after starting ADA or etanercept (ETA). The differential gene expression of M2- and M1-related transcripts was studied in macrophage-derived monocytes after differentiation. Results: At baseline, RA monocytes showed a defect of polarization to M2-like macrophages as compared with healthy donor monocytes, which was negatively correlated with disease activity. M2-like polarization from circulating monocytes was restored only with ADA and not ETA treatment. The transcriptomic signature demonstrated downregulation of M2-related transcripts and upregulation of M1-related transcripts in active RA. In patients receiving ADA, the transcriptomic signature of M2-related transcripts was restored. Conclusion: This longitudinal study demonstrates that ADA but not ETA is able to restore the M2-like polarization of monocytes that is defective in RA.",

keywords = "Adalimumab, Etanercept, M2-like macrophages, monocyte-derived macrophages, rheumatoid arthritis",

author = "Audrey Paoletti and Bineta Ly and Samuel Bitoun and Ga{\"e}tane Nocturne and Elodie Rivi{\`e}re and Manson, {Jessica J.} and Andrea Matucci and Marc Pallardy and {de Vries}, Niek and Xavier Mariette",

note = "Funding Information: This work was supported by the Laboratoire d{\textquoteright}Excellence en Recherche sur le M{\'e}dicament et l{\textquoteright}Innovation Th{\'e}rapeutique (ANR10), Fondation pour la Recherche M{\'e}dicale DEQ20150934719, ABIRISK (Anti-Biopharmaceutical Immunization: prediction and analysis of clinical relevance to minimize the risk), and the Innovative Medicines Initiative Joint Undertaking (grant no. 115303), resources of which are composed of financial contribution from the European Union{\textquoteright}s Seventh Framework Programme (FP7/2007-2013) and EFPIA companies{\textquoteright} in-kind contribution. Funding Information: We thank the steering committee of ABIRISK: M. Pallardy, F. Deisenhammer, J. Davidson, A. Hincelin-Mery, P. D?nnes, A. Fogdell-Hahn, P. Bro?t, X. Mariette, and M. Allez. We would like to thank the clinicians who contributed to the recruitment of patients in the ABIRA prospective study: Olivier Brocq, Princess Grace Hospital, Monaco; Maxime Dougados, APHP h?pital Cochin, Paris; Bruno Fautrel, H?pital Piti?-Salp?tri?re, Paris; Philippe Dieud?, H?pital Bichat, Paris; Francis Berenbaum, H?pital Saint Antoine, Paris; Aleth Pedriger, H?pital Sud, Rennes; Hubert Marotte, CHU de Saint-Etienne, H?pital Nord, Saint-Etienne; Alain Cantagrel and Arnaud Constantin, CHU de Toulouse, Toulouse; Olivier Vittecoq and Thierry Lequere, CHU de Rouen, H?pital Bois Guillaume, Rouen; Alain Saraux, CHU de la Cavale Blanche, Brest; Ren?-Marc Flipo, H?pital Roger Salengro, Lille; Jean Sibilia, CHU de Strasbourg, H?pital de Hautepierre, Strasbourg; Jacques Morel, CHU Lapeyronie, Montpellier; Daniel Wendling, CHRU de Besan?on, Besan?on; Christophe Richez and Thierry Schaeverbeke, H?pital Pellegrin, Bordeaux; and Pascale Vergne-Salle, H?pital Dupuytren, Limoges. We are thankful to Veronique Berthou (Sanofi) for her work in implementing the eCRFs of the ABIRISK prospective studies, to Smail Bouarour (Unit? de recherche clinique, APHP.Universit? Paris-Saclay) for monitoring the study, and to Signe Hassler (CESP, INSERM UMR 1018, Universit? Paris-Saclay) for extraction of clinical data. We thank Aude Gleizes and Salima Hacein-Bey, APHP H?pital Bic?tre, for storage of the samples and lse T.G. Niewold of Rheumatology & Clinical Immunology Amsterdam for sending the samples. We thank Juliette Hamroune, Benjamin Saintpierre and Franck Letourneur of the Universit? de Paris, Institut Cochin, CNRS, INSERM, Plate-Forme S?quen?age et G?nomique (Genom?IC), INSERM U1016, Institut Cochin, 22 rue M?chain, 75014, Paris, France. Publisher Copyright: Copyright {\textcopyright} 2022 Paoletti, Ly, Bitoun, Nocturne, Rivi{\`e}re, Manson, Matucci, Pallardy, De Vries and Mariette.",

year = "2022",

month = feb,

day = "23",

doi = "10.3389/fimmu.2022.832117",

language = "English",

volume = "13",

journal = "Frontiers in Immunology",

issn = "1664-3224",

}

TY - JOUR

T1 - Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis

AU - Paoletti, Audrey

AU - Ly, Bineta

AU - Bitoun, Samuel

AU - Nocturne, Gaëtane

AU - Rivière, Elodie

AU - Manson, Jessica J.

AU - Matucci, Andrea

AU - Pallardy, Marc

AU - de Vries, Niek

AU - Mariette, Xavier

N1 - Funding Information: This work was supported by the Laboratoire d’Excellence en Recherche sur le Médicament et l’Innovation Thérapeutique (ANR10), Fondation pour la Recherche Médicale DEQ20150934719, ABIRISK (Anti-Biopharmaceutical Immunization: prediction and analysis of clinical relevance to minimize the risk), and the Innovative Medicines Initiative Joint Undertaking (grant no. 115303), resources of which are composed of financial contribution from the European Union’s Seventh Framework Programme (FP7/2007-2013) and EFPIA companies’ in-kind contribution. Funding Information: We thank the steering committee of ABIRISK: M. Pallardy, F. Deisenhammer, J. Davidson, A. Hincelin-Mery, P. D?nnes, A. Fogdell-Hahn, P. Bro?t, X. Mariette, and M. Allez. We would like to thank the clinicians who contributed to the recruitment of patients in the ABIRA prospective study: Olivier Brocq, Princess Grace Hospital, Monaco; Maxime Dougados, APHP h?pital Cochin, Paris; Bruno Fautrel, H?pital Piti?-Salp?tri?re, Paris; Philippe Dieud?, H?pital Bichat, Paris; Francis Berenbaum, H?pital Saint Antoine, Paris; Aleth Pedriger, H?pital Sud, Rennes; Hubert Marotte, CHU de Saint-Etienne, H?pital Nord, Saint-Etienne; Alain Cantagrel and Arnaud Constantin, CHU de Toulouse, Toulouse; Olivier Vittecoq and Thierry Lequere, CHU de Rouen, H?pital Bois Guillaume, Rouen; Alain Saraux, CHU de la Cavale Blanche, Brest; Ren?-Marc Flipo, H?pital Roger Salengro, Lille; Jean Sibilia, CHU de Strasbourg, H?pital de Hautepierre, Strasbourg; Jacques Morel, CHU Lapeyronie, Montpellier; Daniel Wendling, CHRU de Besan?on, Besan?on; Christophe Richez and Thierry Schaeverbeke, H?pital Pellegrin, Bordeaux; and Pascale Vergne-Salle, H?pital Dupuytren, Limoges. We are thankful to Veronique Berthou (Sanofi) for her work in implementing the eCRFs of the ABIRISK prospective studies, to Smail Bouarour (Unit? de recherche clinique, APHP.Universit? Paris-Saclay) for monitoring the study, and to Signe Hassler (CESP, INSERM UMR 1018, Universit? Paris-Saclay) for extraction of clinical data. We thank Aude Gleizes and Salima Hacein-Bey, APHP H?pital Bic?tre, for storage of the samples and lse T.G. Niewold of Rheumatology & Clinical Immunology Amsterdam for sending the samples. We thank Juliette Hamroune, Benjamin Saintpierre and Franck Letourneur of the Universit? de Paris, Institut Cochin, CNRS, INSERM, Plate-Forme S?quen?age et G?nomique (Genom?IC), INSERM U1016, Institut Cochin, 22 rue M?chain, 75014, Paris, France. Publisher Copyright: Copyright © 2022 Paoletti, Ly, Bitoun, Nocturne, Rivière, Manson, Matucci, Pallardy, De Vries and Mariette.

PY - 2022/2/23

Y1 - 2022/2/23

N2 - Introduction: We previously reported a specific defect of rheumatoid arthritis (RA) monocyte polarization to anti-inflammatory M2-like macrophages related to increased miR-155 expression in all RA patients except those receiving adalimumab (ADA). In this longitudinal study, we examined whether different tumor necrosis factor inhibitors were able to restore monocyte polarization to M2-like macrophages and their effect on the transcriptomic signature. Methods: M2-like polarization induced by human serum AB was studied in 7 healthy donors and 20 RA patients included in the ABIRA cohort before and 3 months after starting ADA or etanercept (ETA). The differential gene expression of M2- and M1-related transcripts was studied in macrophage-derived monocytes after differentiation. Results: At baseline, RA monocytes showed a defect of polarization to M2-like macrophages as compared with healthy donor monocytes, which was negatively correlated with disease activity. M2-like polarization from circulating monocytes was restored only with ADA and not ETA treatment. The transcriptomic signature demonstrated downregulation of M2-related transcripts and upregulation of M1-related transcripts in active RA. In patients receiving ADA, the transcriptomic signature of M2-related transcripts was restored. Conclusion: This longitudinal study demonstrates that ADA but not ETA is able to restore the M2-like polarization of monocytes that is defective in RA.

AB - Introduction: We previously reported a specific defect of rheumatoid arthritis (RA) monocyte polarization to anti-inflammatory M2-like macrophages related to increased miR-155 expression in all RA patients except those receiving adalimumab (ADA). In this longitudinal study, we examined whether different tumor necrosis factor inhibitors were able to restore monocyte polarization to M2-like macrophages and their effect on the transcriptomic signature. Methods: M2-like polarization induced by human serum AB was studied in 7 healthy donors and 20 RA patients included in the ABIRA cohort before and 3 months after starting ADA or etanercept (ETA). The differential gene expression of M2- and M1-related transcripts was studied in macrophage-derived monocytes after differentiation. Results: At baseline, RA monocytes showed a defect of polarization to M2-like macrophages as compared with healthy donor monocytes, which was negatively correlated with disease activity. M2-like polarization from circulating monocytes was restored only with ADA and not ETA treatment. The transcriptomic signature demonstrated downregulation of M2-related transcripts and upregulation of M1-related transcripts in active RA. In patients receiving ADA, the transcriptomic signature of M2-related transcripts was restored. Conclusion: This longitudinal study demonstrates that ADA but not ETA is able to restore the M2-like polarization of monocytes that is defective in RA.

KW - Adalimumab

KW - Etanercept

KW - M2-like macrophages

KW - monocyte-derived macrophages

KW - rheumatoid arthritis

UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85126260743&origin=inward

UR - https://www.ncbi.nlm.nih.gov/pubmed/35281074

U2 - 10.3389/fimmu.2022.832117

DO - 10.3389/fimmu.2022.832117

M3 - Article

C2 - 35281074

SN - 1664-3224

VL - 13

JO - Frontiers in Immunology

JF - Frontiers in Immunology

M1 - 832117

ER -

Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis

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