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2. Psoriatic arthritis with hyperuricemia: more peripheral, destructive, and challenging to treat

Author

L. Widawski, T. Fabacher, L. Spielmann, JE. Gottenberg, J. Sibilia, PM. Duret, L. Messer, and R. Felten

Subjects
Rheumatology, General Medicine
Abstract

Objective To study the impact of hyperuricemia on clinical presentation, severity, and associated comorbidities of psoriatic arthritis (PsA). Methods Retrospective bicentric case–control study performed in Strasbourg and Colmar, France, from 2009 to 2019. Patients with PsA (according to ICD-10 coding) and at least one available serum urate (SU) measurement were included. Demographic, comorbidities, clinical, and radiographic data were collected. Hyperuricemia was defined as SU level ≥ 360 µmol/L. Results We included 242 patients: 73 (30.2%) had hyperuricemia and 15 (6.2%) met 2015 ACR/EULAR criteria for gout. On univariate analysis, as compared with normo-uricemic patients, hyperuricemic patients were more frequently male (72.6% vs 39.1%, p = 1.6 × 10−6) with higher body mass index (30.9 vs 28.7 kg/m2, p = 0.015) and more comorbidities (Charlson comorbidity index: 2.6 vs 1.8, p = 0.005). PsA started at an older age (47.5 vs 43 years, p = 0.016) was more polyarticular (56.2% vs 41.9%, p = 0.049) than axial (9.6% vs 22.8%, p = 0.019) and more destructive (52.8% vs 37.4%, p = 0.032). PsA patients with joint destruction more frequently had hyperuricemia than did others (37.6% vs 25.8%, p = 0.047). Multivariable analysis confirmed the association of hyperuricemic PsA with peripheral joint involvement (odds ratio 2.98; 95% confidence interval 1.15–7.75; p = 0.025) and less good response to treatment (0.35; 0.15–0.87; p = 0.024). Conclusion Patients with hyperuricemic PsA show poorer response to PsA treatment and have more peripheral and destructive joint damage than normo-uricemic patients. Key Points• Gout and psoriatic arthritis (PsA) can co-exist in the same patient.• Monosodium urate crystals might have a deleterious impact on PsA.• Hyperuricemic PsA is more polyarticular, less frequently axial, and more destructive than normo-uricemic PsA.• PsA with hyperuricemia should lead to more personalized medicine.

Published
2022
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3. Est-il possible d’évaluer la pseudopolyarthrite rhizomélique sans CRP ? Concordance et corrélation entre différents scores d’activité DAS-PPR dans la pseudopolyarthrite rhizomélique

Author

J. D’agostino, A. Saraux, G. Carvajal Alegria, E. Dernis, C. Richez, M.E. Truchetet, D. Wendling, É. Toussirot, A. Perdriger, J.E. Gottenberg, R. Felten, B. Fautrel, L. Chiche, P. Hilliquin, C. Le Henaff, B. Dervieux, G. Direz, I. Chary-Valckenaere, D. Cornec, D. Guellec, T. Marhadour, A. Souki, E. Nowak, and V. Devauchelle Pensec

Subjects
Rheumatology
Published
2022
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5. Facteurs prédictifs d’évolution favorable de la pseudo-polyarthrite rhizomélique corticodépendante

Author

S. Boukhlal, A. Souki, E. Nowak, G. Carvajal Alegria, E. Dernis, C. Richez, G. Direz, I. Chary Valckenaere, M.E. Truchetet, D. Wendling, É. Toussirot, A. Perdriger, J.E. Gottenberg, R. Felten, B. Fautrel, L. Chiche, P. Hilliquin, C. Le Henaff, B. Dervieux, D. Guellec, T. Marhadour, D. Cornec, A. Saraux, and V. Devauchelle Pensec

Subjects
Rheumatology
Published
2022
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10. Efficacité du Tocilizumab chez les patients ayant une Pseudo Polyarthrite Rhizomélique active malgré un traitement par corticothérapie : une étude thérapeutique randomisée

Author

V. Devauchelle Pensec, G. Carvajal Alegria, E. Dernis, C. Richez, M.E. Truchetet, D. Wendling, É. Toussirot, A. Perdriger, J.E. Gottenberg, R. Felten, B. Fautrel, L. Chiche, P. Hilliquin, C. Le Henaff, B. Dervieux, G. Direz, I. Chary Valckenaere, D. Cornec, D. Guellec, T. Marhadour, E. Nowak, and A. Saraux

Subjects
Rheumatology
Published
2022
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12. Coordination régionale et suivi prospectif du traitement prophylactique et curatif de 301 patients traités par anticorps monoclonaux anti-SARS-CoV-2

Author

P. Licinio, M. Weil, M.H. Morel, D. Marin Braun, B. Gourieux, C. Klein, C. Sordet, E. Chatelus, R. Felten, A. Meyer, J. Sibilia, S. Hirschi, T. Degot, B. Renaud Picard, E. Virot, B. Michard, L.D. Kremer, K. Bigault, R. Cevallos, N. Lefebvre, Y. Hansmann, C. Bronner, M.C. Rybarczyk-Vigouret, L. Pain, and J.E. Gottenberg

Subjects
Rheumatology
Published
2022
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14. POS0097 IDENTIFICATION OF NEW CANDIDATE DRUGS FOR PRIMARY SJÖGREN’S SYNDROME USING A DRUG REPURPOSING TRANSCRIPTOMIC APPROACH

Author

R. Felten, T. Ye, C. Schleiss, B. Schwikowski, J. Sibilia, F. Monneaux, H. Dumortier, R. Jonsson, C. Lessard, W. F. Ng, T. Takeuchi, X. Mariette, and J. E. Gottenberg

Subjects
Rheumatology, Immunology, Immunology and Allergy, General Biochemistry, Genetics and Molecular Biology
Abstract

BackgroundNo immunomodulatory drug has ever demonstrated its efficacy in primary Sjögren’s Syndrome (pSS). Drug repurposing, or drug repositioning, refers to the use in another disease of an existing drug, originally approved or evaluated in a different disease.ObjectivesThe objective of our study was to repurpose existing therapeutic drugs in pSS using a transcriptomic approach.MethodsWe generated pSS transcriptomic signatures from peripheral blood samples of patients with pSS compared to healthy controls in two cohorts (ASSESS and a Norwegian cohort) and data mined available pSS transcriptomic signatures in public databases. We compared each disease signature to transcriptomic signatures, obtained from the biological action of 2837 drugs, 2160 knock-in and 3799 knock-down genes, available in the Connectivity Map database. A median similarity score with regard to disease signatures was computed for each candidate drug/gene. Drugs and genes were selected if p│80│. If this score is sufficiently high and statistically significant (>80, pFigure 1.Methods of drug-repurposing transcriptomic analysis (adapted from Toro-Dominguez et al, Arthritis Res Ther 2017;19:54)Results1091 peripheral blood transcriptomes were analyzed from 6 independent studies (906 patients with pSS and 185 healthy controls). Our analysis identified 11 transcriptomic drug signatures significantly associated with pSS signature. We identified 72 transcriptomic knock-in (11) or knock-down (61) gene signatures significantly associated with that of pSS, including 21 with a negative similarity score (Table 1).Table 1.Knock-down and knock-in genes significantly associated with the pSS transcriptomic signaturesType ofexperimentSimilarity scoreGenesNumber of genesKnock-in+IFNG, DUSP28, IFNB1, LYN, BCL2L2, TNFRSF1A, CD40, BCL10, NLK, ZNF39810-SLC52A2111Knock-down+SLC25A14, GOLIM4, DTYMK, DCXR, RRM2, IMPA1, CLTB, F12, CAB39, ID1, ISOC1, UBAP1, HIGD2A, UFD1L, SOD2, BTG1, PRKCI, HIST2H2BE, NISCH, TEAD4, MTX2, TYK2, GTF2B, NDUFS7, NNT, ACADSB, GSTP1, HOMER2, SORBS3, PCK2, PHB2, PDXK, TES, TM9SF2, TBX2, HOXA6, KIF2C, MED1, NR2F6, CD14, BECN141-TM9SF3, E2F3, PRMT3, KD, PKN2, SUCLA2, CD44, GRN, SP3, ATP5S, MYCBP2, TRAF7, POLA2, ADRB2, PSMG1, PPP2R3C, PMAIP1, ETFA, ANKRD37, SPECC1L2061Type I and II interferons were highly ranked (similarity score >99), and their overexpression mimicked the disease signature. CD40 appeared also as a very relevant target (similarity score = 98.8). Three drugs had a significant negative similarity score: ampicillin (-88.69, p=0.0019), amylocaine (-88.28, p=0.0026), and droxinostat (-85.42, p=0.0027). Droxinostat is a HDAC inhibitor. HDAC activity has been shown to be an essential element of the coactivation system for IFN-induced gene regulation and the IFN-induced innate immune response.ConclusionThis first drug repositioning transcriptomic approach in Sjögren’s syndrome confirms the interest of targeting interferons and identifies histone deacetylases as potential therapeutic targets.AcknowledgementsInvestigators of the ASSESS cohort: Emmanuelle Dernis, Valerie Devauchelle-Pensec, Philippe Dieude, Jean-Jacques Dubost, Anne-Laure Fauchais, Vincent Goeb, Eric Hachulla, Pierre Yves Hatron, Claire Larroche, Véronique Le Guern, Jacques Morel, Aleth Perdriger, Carinne Salliot, Stephanie Rist, Alain Saraux, Jean Sibilia, Olivier Vittecoq, Gaétane Nocturne, Philippe Ravaud, Raphaèle SerorCentre de Ressources Biologiques de l’Hôpital Bichat: Sarah TubianaJohan G. Brun for contributing to the Norwegian cohort.Funding SourcesThis work was supported by the Innovative Medicines Initiative 2 Joint Undertaking (IMI 2 JU) (NECESSITY grant 806975). The Joint Undertaking received support from the European Union’s Horizon 2020 Research and Innovation Program and from the European Federation of Pharmaceutical Industries and Associations. This work was also supported by R01 AR065953 Beth the NIH, United States. The contents are the sole responsibility of the authors and do not necessarily the official views of the NIH.JEG received an unrestricted grant from Bristol-Myer-Squibbs to do the transcriptomic analysis of the ASSESS and Norwegian cohorts. JEG received a grant from Geneviève Garnier (Association Française du Syndrome de Gougerot-Sjögren et des syndromes secs).The ASSESS cohort is promoted by the French Society of Rheumatology and received two research grants from the French Society of Rheumatology.The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.Disclosure of InterestsRenaud FELTEN: None declared, Tao Ye: None declared, Cédric Schleiss: None declared, Benno Schwikowski: None declared, Jean Sibilia: None declared, Fanny Monneaux: None declared, Hélène Dumortier: None declared, Roland Jonsson: None declared, Christopher Lessard: None declared, Wan Fai Ng: None declared, Tsutomu Takeuchi: None declared, Xavier Mariette: None declared, Jacques-Eric Gottenberg Grant/research support from: JEG received an unrestricted grant from Bristol-Myer-Squibbs to do the transcriptomic analysis of the ASSESS and Norwegian cohorts.

Published
2022
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15. Psoriatic arthritis with hyperuricemia: more peripheral, destructive, and challenging to treat

Author

L, Widawski, T, Fabacher, L, Spielmann, J E, Gottenberg, J, Sibilia, P M, Duret, L, Messer, and R, Felten

Subjects
Gout, Case-Control Studies, Arthritis, Psoriatic, Humans, Hyperuricemia, Retrospective Studies
Abstract

To study the impact of hyperuricemia on clinical presentation, severity, and associated comorbidities of psoriatic arthritis (PsA).Retrospective bicentric case-control study performed in Strasbourg and Colmar, France, from 2009 to 2019. Patients with PsA (according to ICD-10 coding) and at least one available serum urate (SU) measurement were included. Demographic, comorbidities, clinical, and radiographic data were collected. Hyperuricemia was defined as SU level ≥ 360 µmol/L.We included 242 patients: 73 (30.2%) had hyperuricemia and 15 (6.2%) met 2015 ACR/EULAR criteria for gout. On univariate analysis, as compared with normo-uricemic patients, hyperuricemic patients were more frequently male (72.6% vs 39.1%, p = 1.6 × 10Patients with hyperuricemic PsA show poorer response to PsA treatment and have more peripheral and destructive joint damage than normo-uricemic patients. Key Points • Gout and psoriatic arthritis (PsA) can co-exist in the same patient. • Monosodium urate crystals might have a deleterious impact on PsA. • Hyperuricemic PsA is more polyarticular, less frequently axial, and more destructive than normo-uricemic PsA. • PsA with hyperuricemia should lead to more personalized medicine.

Published
2021

16. POS1065 IMPACT OF HYPERURICEMIA ON CLINICAL PHENOTYPE, COMORBIDITIES, AND RESPONSE TO SECUKINUMAB IN PSORIATIC ARTHRITIS: POST HOC ANALYSIS OF FUTURE AND MAXIMISE STUDIES

Author

R. Felten, L. Widawski, L. Spielmann, C. Gaillez, W. Bao, J. E. Gottenberg, P. M. Duret, and L. Messer

Subjects
Rheumatology, Immunology, Immunology and Allergy, General Biochemistry, Genetics and Molecular Biology
Abstract

BackgroundHyperuricemia (HU) is a metabolic abnormality associated with psoriasis (PsO) and psoriatic arthritis (PsA)1. The prevalence of HU is 2–13% in general population, 19–20% in PsO patients (pts), and 27–32% in PsA pts1,2. Pts with PsO/PsA are at significantly increased risk of HU and development of gout1. The pathogenic role of chronic HU in the development and maintenance of PsA is based on epidemiological, clinical, and fundamental arguments and hence does not appear fortuitous. These processes can influence each other3. Moreover, PsA with HU has been shown to be more peripheral, destructive, and challenging to treat4.ObjectivesTo evaluate the impact of HU on PsA in terms of clinical presentation, severity, comorbidities, and response to secukinumab (SEC) over 1-year.MethodsThis post hoc analysis included pooled data from PsA pts enrolled in the FUTURE 2–5 and MAXIMISE phase 3 trials. Pts were stratified into 2 groups based on baseline (BL) serum uric acid (SUA) level (HU: ≥360 µmol/L; without HU: ResultsOverall, 2504 PsA pts were included in the analysis, of which 822 (32.8%) had HU (62 [2.5%] with gout; 49 [2.0%] treated with ULT). At BL, pts with HU were mostly male (76.0% vs 34.2%) and had a higher body mass index (30.9 vs 28.3 kg/m2) with more comorbidities, such as hypertension (43.8% vs 31.3%), compared to pts without HU. A higher proportion of pts with HU had dactylitis (34.5% vs 25.9%), and PsO (48.3% vs 36.3%) with a greater mean PASI score (13.6 vs 10.2), compared to pts without HU (Table 1). The proportion of pts achieving ACR50, resolution of enthesitis/dactylitis, and mean change in HAQ-DI score were comparable up to Week 52 irrespective of BL HU status. The PASI90 response rate was higher in pts without HU with SEC 150 mg (with and without load) and similar in SEC 300 mg group irrespective of BL HU status (Figure 1).Table 1.Demographics and baseline characteristicsParameters, mean ± SD unless specifiedWith hyperuricemia (N=822)Without hyperuricemia (N=1682)Age (Years)48.5 ± 12.4148.3 ± 12.19Gender (Male), n (%)625 (76.0)576 (34.2)Weight (kg)92.71 ± 18.6279.59 ± 17.55BMI (kg/m2)30.90 ± 5.8628.33 ± 5.91History of hypertension, n (%)360 (43.8)526 (31.3)History of diabetes mellitus, n (%)85 (10.3)144 (8.6)TJC20.6 ± 15.5221.3 ± 16.25SJC10.9 ± 9.3110.8 ± 9.13Enthesitis, n (%)412 (50.1)852 (50.7)Dactylitis, n (%)284 (34.5)436 (25.9)Evidence of current psoriasis; n (%)397 (48.3)611 (36.3)Mean PASI score*13.61 ± 11.0310.16 ± 9.13TNFi naїve, n (%)477 (58.0)938 (55.8)MTX use at randomization, n (%)321 (39.1)685 (40.7)Serum uric acid (µmol/L)420.7 ± 57.11274.9 ± 51.98CRP (mg/L)11.6 ± 18.6610.7 ± 23.36*not collected in MAXMISEBMI, body mass index; CRP, C-reactive protein; MTX, methotrexate; SJC, swollen joint count; TJC, tender joint count; TNFi, tumor necrosis factor inhibitorConclusionIn this pooled analysis of SEC PsA studies, pts with HU reported a higher prevalence of hypertension, with more clinical dactylitis, and more PsO, with higher PASI score compared to pts without HU. Efficacy across all musculoskeletal manifestations was similar with SEC 150 and 300 mg; while PASI90 response rate was slightly better in patients without HU with SEC 150 mg, and similar with SEC 300 mg irrespective of HU status, at 1-year.References[1]Tripolino C, et al. Front Med. 2021;8:737573[2]AlJohani R, et al. J Rheumatol. 2018;45(2):213–7[3]Felten R, et al. Clin Rheumatol. 2020;39:1405–13[4]Widawski L, et al. Clin Rheumatol. 2022. https://doi.org/10.1007/s10067-022-06061-xDisclosure of InterestsRenaud FELTEN Consultant of: Novartis (Advisory board), Laura Widawski: None declared, Lionel Spielmann: None declared, Corine Gaillez Shareholder of: Novartis, Employee of: Novartis, Weibin Bao Shareholder of: Novartis, Employee of: Novartis, Jacques-Eric Gottenberg Consultant of: Novartis (Advisory board), Pierre-Marie Duret: None declared, Laurent Messer: None declared

Published
2022
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17. POS0711 TOLERANCE AND EFFICACY OF TARGETED THERAPIES PRESCRIBED FOR OFF-LABEL INDICATIONS IN REFRACTORY SYSTEMIC AUTOIMMUNE DISEASES: DATA OF THE FIRST 100 PATIENTS ENROLLED IN THE TATA REGISTRY (TARGETED THERAPY IN AUTOIMMUNE DISEASES)

Author

J. E. Gottenberg, A. Chaudier, Y. Allenbach, A. Mekinian, Z. Amoura, P. Cacoub, D. Cornec, E. Hachulla, P. Quartier, I. Melki, C. Richez, R. Seror, B. Terrier, V. Devauchelle-Pensec, J. Henry, M. Gatfosse, L. Bouillet, E. Gaigneux, V. Andre, G. Baulier, A. Saunier, M. Desmurs, A. Poulet, M. Ete, M. E. Truchetet, M. Michaud, C. Larroche, A. Dellal, A. Leurs, S. Ottaviani, H. Nielly, G. Vial, R. Jaussaud, B. Rouviere, P. Y. Jeandel, A. Guffroy, A. S. Korganow, M. Jouvray, A. Meyer, E. Chatelus, C. Sordet, R. Felten, J. Sibilia, S. Ahmed Yahia, J. F. Kleinmann, and X. Mariette

Subjects
Rheumatology, Immunology, Immunology and Allergy, General Biochemistry, Genetics and Molecular Biology
Abstract

BackgroundThe low prevalence of systemic autoimmune diseases and the diversity of their clinical manifestations make complex to conduct randomised clinical trials to assess the potential efficacy of targeted treatments.ObjectivesTo assess the tolerance and efficacy of targeted therapies prescribed off-label in refractory autoimmune diseases.MethodsThe TATA registry (TArgeted Therapy in Autoimmune Diseases) is a prospective, observational, national and independent cohort follow-up. The inclusion criteria in the registry are as follows: age > 18 years; rare systemic autoimmune disease (systemic lupus erythematosus, Sjögren’s syndrome, systemic scleroderma, inflammatory myopathy, vasculitis) or other refractory rheumatism treated with off-label drugs started after 1st January 2019.ResultsHundred (100) patients (79 females) were enrolled. The median age was 52.5 years [49;56], the median disease duration before enrolment was 5 years [3;7]. The targeted therapies at enrolment were as follows: JAK/STAT inhibitors (44%), anti-IL6R (22%), anti-IL12/23, anti-IL23 and anti-IL17 (9%), anti-BAFF (5%), abatacept (5%), other targeted treatments (9%), and combination of targeted treatments (6%). 73% of patients were receiving corticosteroid therapy at enrolment (median dose 10 mg/day). The current median follow-up time is 9 months [8;10].Safety: 11 serious infections (incidence rate of 14.8 /100 patient-years) and 1 cancer (1.3 cancers/100 patient-years) were observed. Two patients died from severe COVID-19 (2.7 deaths/100 patient-years).Efficacy: The targeted treatment was considered effective by the clinician in 56% of patients and allowed in responders a median reduction of oral corticosteroids of 15 [9-21] mg/day.ConclusionThese initial results of the TATA registry confirm the diversity of targeted treatments prescribed off-label in refractory autoimmune diseases and their corticosteroid-sparing effect when effective. Tolerance was acceptable in these refractory patients with a long history of treatment with immunosuppressive drugs.References[1]B. Terrier et al., Safety and efficacy of rituximab in systemic lupus erythematosus: results from 136 patients from the French AutoImmunity and Rituximab registry. Arthritis Rheum 62, 2458-2466 (2010).[2]J. E. Gottenberg et al., Efficacy of rituximab in systemic manifestations of primary Sjogren’s syndrome: results in 78 patients of the AutoImmune and Rituximab registry. Ann Rheum Dis 72, 1026-1031 (2013).[3]J. E. Gottenberg et al., Risk factors for severe infections in patients with rheumatoid arthritis treated with rituximab in the autoimmunity and rituximab registry. Arthritis Rheum 62, 2625-2632 (2010).[4]F. R. S. S. S. C. I. consortium, contributors, Severity of COVID-19 and survival in patients with rheumatic and inflammatory diseases: data from the French RMD COVID-19 cohort of 694 patients. Ann Rheum Dis, (2020).[5]R. Felten et al., B-cell targeted therapy is associated with severe COVID-19 among patients with inflammatory arthritides: a 1-year multicentre study in 1116 successive patients receiving intravenous biologics. Ann Rheum Dis 81, 143-145 (2022).[6]D. J. Wallace et al., Baricitinib for systemic lupus erythematosus: a double-blind, randomised, placebo-controlled, phase 2 trial. Lancet 392, 222-231 (2018).[7]J. J. Paik et al., Study of Tofacitinib in Refractory Dermatomyositis: An Open-Label Pilot Study of Ten Patients. Arthritis Rheumatol 73, 858-865 (2021).[8]S. Cole et al., Integrative analysis reveals CD38 as a therapeutic target for plasma cell-rich pre-disease and established rheumatoid arthritis and systemic lupus erythematosus. Arthritis Res Ther 20, 85 (2018).[9]S. J. Bowman et al., Safety and efficacy of subcutaneous ianalumab (VAY736) in patients with primary Sjogren’s syndrome: a randomised, double-blind, placebo-controlled, phase 2b dose-finding trial. Lancet 399, 161-171 (2022).AcknowledgementsFrench networks (FAI2R, CRI, IMIDIATE, SFR, SNFMI) focused on rare systemic autoimmune diseases contributed this work by the contribution of network-affiliated physicians.Disclosure of InterestsJacques-Eric Gottenberg Consultant of: Abbvie, BMS, Gilead, Galapagos, Novartis, Lilly Roche Chugai, Sanofi, Janssen, Pfizer, Grant/research support from: BMS.Lilly and Pfizer for this register (with no access to data)., Aurore Chaudier: None declared, Yves Allenbach: None declared, Arsene Mekinian: None declared, Zahir Amoura: None declared, Patrice cacoub: None declared, Divi Cornec: None declared, Eric Hachulla: None declared, Pierre Quartier: None declared, isabelle melki: None declared, Christophe Richez: None declared, Raphaèle Seror: None declared, Benjamin Terrier: None declared, Valerie Devauchelle-Pensec: None declared, Julien Henry: None declared, MARC GATFOSSE: None declared, LAURENCE BOUILLET: None declared, Emeline GAIGNEUX: None declared, Vincent ANDRE: None declared, Gildas BAULIER: None declared, Aurélie SAUNIER: None declared, Marie Desmurs: None declared, Antoine POULET: None declared, Mathieu ETE: None declared, Marie-Elise Truchetet: None declared, Martin Michaud: None declared, Claire Larroche: None declared, AZEDDINE DELLAL: None declared, Amelie LEURS: None declared, Sebastien Ottaviani: None declared, Hubert NIELLY: None declared, Guillaume VIAL: None declared, Roland JAUSSAUD: None declared, Benedicte ROUVIERE: None declared, Pierre-Yves JEANDEL: None declared, Aurelien GUFFROY: None declared, Anne-Sophie Korganow: None declared, Mathieu JOUVRAY: None declared, alain meyer: None declared, Emmanuel Chatelus: None declared, Christelle Sordet: None declared, Renaud FELTEN: None declared, Jean Sibilia: None declared, Samira AHMED YAHIA: None declared, Jean François Kleinmann: None declared, Xavier Mariette Consultant of: BMS, Galapagos, GSK, Janssen, Novartis, Pfizer, Sanofi, UCB

Published
2022
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18. POS1223 DIFFERENT ANTI-SARS-CoV-2 VACCINE RESPONSE UNDER B- AND T-CELL TARGETED THERAPIES VERSUS ANTI-CYTOKINE THERAPIES IN PATIENTS WITH INFLAMMATORY ARTHRITIDES

Author

R. Felten, M. Geoffroy, B. Loïs, P. M. Duret, M. Desmurs, A. Fan, M. Couderc, L. Messer, M. Ardizzone, S. Ahmed-Yahia, R. M. Javier, A. Meyer, E. Chatelus, C. Sordet, L. Pijnenburg, J. Sibilia, M. Soubrier, J. E. Gottenberg, and J. H. Salmon

Subjects
Rheumatology, Immunology, Immunology and Allergy, General Biochemistry, Genetics and Molecular Biology
Abstract

BackgroundVaccination against SARS-CoV-2 is effective in preventing severe forms of COVID-19, but there remain concerns about a reduced vaccine response in patients suffering from inflammatory arthritides who are treated by immunosuppressive therapies.ObjectivesWe analysed the impact of bDMARDs on the humoral anti-SARS-CoV-2 vaccine response of patients followed in day hospitals.MethodsWe studied the vaccine response after a complete vaccine regimen followed in day hospital in 5 French hospitals and treated with an intravenous bDMARD between September 2019 and August 2021. After obtaining their informed consent, we included patients with an anti-SARS-CoV-2 serology. They were considered non-responders if the antibody level detected was inferior to the threshold of positivity of the kit used.Results205 patients were included (148 females/57 males). The median age was 64 years (Interquartile Range [IQR] 56-71). 25 were treated with tocilizumab (TCZ), 36 with abatacept (ABA), 53 with infliximab (IFX) and 91 with rituximab (RTX). When considering both patients after a complete vaccination schema (2 doses, or 1 dose in case of prior COVID-19) and those with 1 booster dose, 34 patients (16.6%) were non-responders (2 [5.9%] treated by IFX, none treated by TCZ, 9 [26.5%] treated by ABA and 23 [67.7%] treated by RTX). In multivariate analysis, the only characteristics that significantly and independently differed between responders and non-responders were last bDMARD and corticosteroid therapy at the time of 1st vaccination (Table 1). In RTX-treated patients, the delay from last infusion to 1st vaccine dose was significantly shorter in non-responders (median 4.3 IQR [2.9-6.1] months in non-responders versus 8.4 IQR [5.7-14.5] in responders, p=0.0007). Median survival, i.e. achieving a vaccine response in 50% of RTX-treated subjects, was achieved after 277 days (95CI [209-310]) in patients vaccinated with 2 or 3 doses (Figure 1). In ABA-treated patients, the delay from last infusion to 1st vaccine dose was not different between non-responders and responders.Table 1.Patients’ characteristics and comparisons between responders and non-responders.All patients (n=205)Responders (n=171)Non responders (n=34)Univariate p valueMultivariatep valueAge (median [IQR]), in years64 [56-71]64 [54-70]69 [57-75.5]0.070.40Female sex, n (%)148 (72.2)125 [73.1)23 (67.7)0.53Inflammatory arthritides, n (%)0.16**0.24 Rheumatoid Arthritis156 (78.0)128 (74.9)28 (82.4)0.51 Spondyloarthritis33 (16.1)31 (18.1)2 (5.9)0.12 Others*16 (7.8)12 (5.9)4 (1.9)0.31Last bDMARDs at time of 1st vaccination, n (%)0.0004ABA/RTX versus IFX/TCZ < 0.00010.00024 Infliximab53 (25.9)51 (29.8)2 (5.9) Tocilizumab25 (12.2)25 (14.6)0 Abatacept36 (17.6)27 (15.8)9 (26.5) Rituximab91 (44.4)68 (39.8)23 (67.7)Associated treatments at time of 1st vaccination CsDMARDs, n (%)126 (61.5)107 (62.6)19(55.9)0.56 Methotrexate91 (44.4)78 (45.6)13 (38.2)0.46 Median dose in users (mg /week) [IQR]15 [10-17.5]13.8 [10-15.6]15 [13.8-20]0.07 Corticosteroids, n (%)25 (12.2)19 (11.1)6 (17.6)0.29 Median dose (mg /day) [IQR]0 [0-0]0 [0-0]0 [0-2]0.0350.016Previous COVID-19 infection, n (%)23 (11.2)21 (12.3)2 (5.9)0.38Type of vaccine, n (%)0.62 Pfizer169 (82.4)142 (83.0)27 (79.4)0.62 Moderna14 (68.3)11 (6.4)3 (8.8)0.71 Astra-Zeneca17 (8.3)15 (8.8)2 (5.9)0.74 Janssen5 (2.4)3 (1.8)2 (5.9)0.19Vaccination, n (%) Complete167 (81.5)141 (82.5)28 (16.8)0.47 Complete + 1 booster dose56 (27.3)43 (25.1)13 (38.2)0.14Figure 1.Cumulative seropositive rate according to the interval (days) between the last course of rituximab administration and vaccinationConclusionABA and RTX alter the anti-SARS-CoV-2 vaccine response and were associated with nearly all vaccine non-responses in the present study. Corticosteroid therapy was associated with a lower vaccine response regardless of its indication or the concomitant use of bMARD.Disclosure of InterestsNone declared

Published
2022
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19. POS0533 REPURPOSING FIB-4 SCORE IN RHEUMATOID ARTHRITIS: DATA FROM THE ESPOIR COHORT

Author

R. Felten, T. Fabacher, N. Sedmak, F. Berenbaum, B. Combe, J. Sibilia, C. Sordet, E. Chatelus, A. Ruyssen-Witrand, O. Vittecoq, N. Meyer, and J. E. Gottenberg

Subjects
Rheumatology, Immunology, Immunology and Allergy, General Biochemistry, Genetics and Molecular Biology
Abstract

BackgroundThe Fibrosis-4 (FIB4) score, including age, transaminases and platelets, can detect severe fibrosis (F3-F4) in patients with Non Alcoolic Steato Hepatitis (NASH) and could be of interest in the follow-up of patients with RA. Indeed, platelets contribute to the pathophysiology of RA, transaminases are used in the liver monitoring of our treatments. In addition, retrospective data suggested the association between FIB4 and mortality in RA (1).ObjectivesWe aimed to evaluate the value of the FIB4 score as a prognostic factor in RA in the prospective ESPOIR cohort.MethodsPatients of the ESPOIR cohort diagnosed with RA according to ACR-EULAR criteria were included in our analysis. The formula for the FIB-4 score is as follows: [Age (years) × ASAT (U/L)] / [Platelet count (10^9/L) × ALT (U/L)1/2]. The analyses were based on linear mixed-effects models with a random effect on the subject to account for repeated measures throughout time.Results633 of the 813 patients included met the ACR/EULAR criteria for RA and had a calculable FIB4 score. Median FIB4 was 0.75 IQR (0.53-0.99) and 61 patients (9.6%) had a high FIB4 score at baseline. Baseline FIB4 was significantly higher in patients with a chronic alcohol consumption (p=0.021) or viral hepatitis (pTable 1.Associations of FIB4 score with DAS28 and modified Sharp score evolutions in multivariate analysesVariableVariables included in modelp-valueDAS28TimeAge0.97Baseline number of swollen jointsBaseline Rheumatoid Factor0.51evolution over timeBaseline ACPA (presence)0.97Baseline CRPBaseline modified Sharp score > 00.15Baseline FIB40.26Modified Sharp scoreTime0.052Age0.0005Baseline number of swollen joints0.38Baseline Rheumatoid Factor0.61evolution over timeBaseline ACPA (presence)0.012Baseline CRP0.84Baseline FIB40.25ConclusionOur study was the first to evaluate the value of FIB4 in a prospective cohort of RA patients. The present prospective cohort study with a 10-year follow-up did not find a prognostic role of FIB4 in RA, in contrast to previous retrospective studies. Reassuringly, FIB4 score was not increased by DMARD treatment after 10 years of follow-up, confirming the absence of long-term DMARD-related hepatotoxicity.References[1]Seung Up Kim, Beom Kyung Kim, Jun Yong Park, Do Young Kim, Sang Hoon Ahn, Yong-Beom Park, Kwang-Hyub Han & Sang-Won Lee (2018): Fibrosis-4 index at diagnosis can predict all-cause mortality in patients with rheumatoid arthritis: A retrospective monocentric study, Modern Rheumatology, DOI: 10.1080/14397595.2018.1558760Figure 1.Impact of baseline FIB4 score on DAS28, HAQ and total modified-Sharp score over time.AcknowledgementsAn unrestricted grant from Merck Sharp and Dohme (MSD) was allocated for the first 5 years. Two additional grants from INSERM were obtained to support part of the biological database. The French Society of Rheumatology, Pfizer, Abbvie, Lilly, Sanofi also supported the ESPOIR cohort study.We also wish to thank Nathalie Rincheval (CHU Montpellier and EA 2415) who did expert monitoring and data management and all the investigators who recruited and followed the patients (F. Berenbaum, Paris-Saint Antoine, MC. Boissier, Paris-Bobigny, A. Cantagrel, Toulouse, B. Combe, Montpellier, M. Dougados, Paris-Cochin, P. Fardellone et P. Boumier Amiens, B. Fautrel, Paris-La Pitié, RM. Flipo, Lille, Ph. Goupille, Tours, F. Liote, Paris- Lariboisière, O. Vittecoq, Rouen, X. Mariette, Paris Bicetre, P. Dieude, Paris Bichat, A. Saraux, Brest, T. Schaeverbeke, Bordeaux, J. Sibilia, Strasbourg) V. Devauchelle and C Lukas for expert X-ray reading.Disclosure of InterestsNone declared.

Published
2022
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20. Acceptabilité de la vaccination contre la Covid-19 chez les patients atteints de maladies rhumatismales chroniques et les professionnels de santé

Author

Mervat Eissa, Nelly Ziade, Basel Masri, M. Metawee, N. Abdullateef, L. El Kibbi, A. Adnan, A. Abi Najm, Hussein Halabi, Wafa Hamdi, M. Elrakawi, F. Abutiban, L. Arnaud, Ihsane Hmamouchi, and R. Felten

Subjects
Rheumatology, Pe.160
Abstract

Introduction Les premiers vaccins contre la COVID-19 ont été autorisés pour utilisation en décembre 2020. Cependant, leur acceptabilité reste controversée. Les objectifs de cette étude étaient d’estimer l’acceptabilité de la vaccination contre la COVID-19 chez les patients atteints de maladies rhumatismales chroniques et les professionnels de santé, et d’évaluer les facteurs associés à cette acceptabilité. Patients et méthodes L’étude ARCOVAX (Etude de la Ligue Arabe des Associations pour la Rhumatologie [ArLAR] sur la vaccination contre la COVID-19) a utilisé un questionnaire anonyme en ligne adapté de l’étude VAXICOV [1], traduit en arabe par les auteurs et validé par le comité scientifique de l’ArLAR. L’enquête a été diffusée en ligne en trois langues : arabe, anglais et français entre le 13 avril et le 11 mai 2021, à travers les réseaux sociaux (Facebook, Twitter, Instagram, Snapchat, Messenger), des associations de patients, des courriels envoyés de la part de l’ArLAR et du groupe AAAA (Arab Adult Arthritis Awareness), des messages WhatsApp aux patients et aux médecins, et des invitations aux patients en utilisant un code QR affiché dans la salle d’attente. L’acceptabilité a été définie par : les participants déjà vaccinés ou désireux de se faire vacciner ; la non-acceptabilité a été définie par : les participants indécis ou refusant de se faire vacciner. Les données démographiques et de la maladie, les perceptions concernant les vaccins contre la COVID-19 ont été recueillies. Les facteurs associés à l’acceptabilité ont été analysés par deux modèles de régression logistique distincts pour les patients et les professionnels de santé. Résultats L’analyse a inclus 3176 participants de 19 pays Arabes (1594 patients et 1517 professionnels de santé). L’âge moyen des patients était de 39 ans, 73 % étaient des femmes et 18 % avaient une éducation universitaire. Vingt-neuf pour cent des patients étaient déjà vaccinés, contre 59 % des professionnels de santé. L’acceptabilité était significativement plus faible chez les patients (63 %) par rapport aux professionnels de santé (81 %), p

Published
2021
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22. [A review of avascular necrosis, of the hip and beyond]

Author

L, Pijnenburg, R, Felten, and R-M, Javier

Subjects
Extracorporeal Shockwave Therapy, Femur Head Necrosis, Risk Factors, Arthroplasty, Replacement, Hip, Humans, Decompression, Surgical, Prognosis
Abstract

Avascular necrosis is an ischemic or cytotoxic necrosis of epiphyseal bone, responsible for joint pain, altered life quality and frequently affecting young patients. Avascular necrosis can be unifocal or multifocal, underlining the possibility of a systemic origin. Avascular necrosis involves the femoral head in more than 75% of cases. Although avascular necrosis is irreversible, many risk factors must be sought, including corticosteroid treatment, hypercholesterolemia, sickle cell disease or alcohol abuse. MRI imaging is the main exploration for the diagnostic and staging of the disease, and should be performed in unexplained hip pain in young patients with normal X-rays. In the earlier stages of the disease (stage I and II of the Arlet and Ficat classification), joint surface is preserved, and conservative treatment is recommended. In the more advanced stages (III and IV of the Arlet and Ficat classification), the articular surface collapses and joint arthroplasty is the main treatment. However, there are some recent therapeutic advances, based on mesenchymal stem cells, which may contribute, in the future, to improve the bad functional prognosis of the disease.

Published
2019

23. OP0130 COMPOSITE OF RELEVANT ENDPOINTS IN SJÖGREN’S SYNDROME (CRESS): A COMPREHENSIVE TOOL FOR CLINICAL TRIALS

Author

S. Arends, L. de Wolff, J. F. Van Nimwegen, G. M. Verstappen, J. Vehof, M. Bombardieri, S. J. Bowman, E. Pontarini, A. Baer, M. Nys, J. E. Gottenberg, R. Felten, N. Ray, A. Vissink, F. G. M. Kroese, and H. Bootsma

Subjects
medicine.medical_specialty, business.industry, Abatacept, Immunology, Placebo, General Biochemistry, Genetics and Molecular Biology, Treatment efficacy, Clinical trial, Rheumatology, Internal medicine, medicine, Clinical endpoint, Immunology and Allergy, Active treatment, Sjogren s, Tear gland, business, medicine.drug
Abstract

Background:Several large randomised controlled trials (RCTs) in primary Sjögren’s syndrome (pSS) failed to demonstrate drug efficacy.1-4 Many of these trials used ESSDAI as primary endpoint, showing large but similar response rates in active treatment and placebo groups.1,3,4 Given the heterogeneous nature of pSS, there is need for a composite endpoint including multiple clinically relevant parameters.Objectives:To develop and validate the Composite of Relevant Endpoints in Sjögren’s Syndrome (CRESS).Methods:A multidisciplinary team of pSS experts selected clinically relevant items and measurements to include in the CRESS. Definition of response of CRESS items was based on clinical relevance, previously defined minimal clinically important improvement (MCII) and data of the single-centre ASAP-III (abatacept) trial.1 CRESS was validated in three independent RCTs: TRACTISS (rituximab) trial2, multi-centre abatacept trial3 and ETAP (tocilizumab) trial4. CRESS response rates were assessed at the primary endpoint visit of all four trials.Results:Five complementary items were selected to form CRESS: systemic disease activity, patient-reported symptoms, tear gland, salivary gland and serological item. Definition of response per item is presented in Table 1. Total CRESS response was defined as response on ≥3 of 5 items. Since not all trials have ocular staining score or salivary gland ultrasonography (SGUS) available, the concise CRESS (cCRESS) was developed simultaneously, leaving Schirmer’s test and unstimulated whole saliva flow for the tear and salivary gland items, respectively. In the ASAP-III trial, CRESS response rates were 24/40 (60%) for abatacept vs. 7/39 (18%) for placebo at week 24 (pTable 1.CRESS items and definition of responseItemsMeasurementsDefinition of responseSystemic disease activityClinESSDAIScorePatient-reported symptomsESSPRIDecrease of ≥1 point or ≥15%Tear gland*Schirmer/OSS**-If abnormal Schirmer (≤5 mm) at baseline: increase of ≥5 mm in Schirmer-Or if abnormal OSS (≥3 points) at baseline: decrease ≥2 points in OSS-Or if both Schirmer/OSS normal scores at baseline: no change to abnormal in bothSalivary gland*UWS/SGUSIncrease of ≥25% in UWS (or if score is 0 at baseline, any increase)Or decrease of ≥25% in total Hocevar score (SGUS)SerologicalRF/IgGDecrease of ≥25% in RFOr decrease of ≥10% in IgGCRESS responderResponder on ≥3 of 5 itemsOcular Staining Score (OSS), Unstimulated whole salivary flow (UWS), Salivary gland ultrasonography (SGUS), Rheumatoid factor (RF), Immunoglobuline G (IgG)*Concise CRESS (cCRESS): CRESS without OSS and SGUS, leaving Schirmer and UWS for tear and salivary gland items, respectively**Mean of both eyesIn the external validation trials, cCRESS response rates for TRACTISS were: 33/67 (49%) rituximab vs. 20/66 (30%) placebo at week 48 (p=0.026). CRESS response rates (without SGUS) for the multi-centre abatacept trial were: 41/92 (45%) abatacept vs. 30/95 (32%) placebo at week 24 (p=0.067). cCRESS response rates (without rheumatoid factor) for ETAP were: 10/55 (18%) tocilizumab vs. 13/55 (24%) placebo at week 24 (p=0.482) (Figure 1A-D). Compared to ESSDAI MCII of ≥3 points decrease, CRESS was able to approximately halve placebo response rates in RCTs with high baseline ESSDAI scores (>5) (Figures 1E-H).Conclusion:CRESS shows lower placebo response rates compared to ESSDAI MCII, which is crucial for demonstrating treatment efficacy. With the CRESS, higher response rates in abatacept and rituximab treated patients compared to placebo were found in RCTs which previously showed negative primary endpoint results. CRESS confirmed that no differences were found for almost all outcome measures between tocilizumab and placebo,4 with low response rates. The CRESS is a well-balanced, feasible, composite endpoint for use in clinical trials in pSS patients.References:[1]Van Nimwegen 2020;9913(19):1–11[2]Bowman 2017;69(7):1440–50[3]Baer (doi:218599)[4]Felten (doi:21846)Acknowledgements:The authors would like to acknowledge all contributors of the included trials.Disclosure of Interests:Suzanne Arends: None declared, Liseth de Wolff: None declared, Jolien F. van Nimwegen Speakers bureau: Bristol Myers Squibb, Consultant of: Bristol Myers Squibb, Gwenny M. Verstappen: None declared, Jelle Vehof: None declared, Michele Bombardieri Consultant of: MedImmune, GlaxoSmithKline, Grant/research support from: MedImmune, Simon J. Bowman Consultant of: AstraZenecea/MedImmune, Bristol Myers Squibb, Celgene, Eli Lilly, Glenmark, GlaxoSmithKline, MTPharma, Novartis, Ono, Pfizer, Takeda, UCB, XTLBio, Elena Pontarini: None declared, Alan Baer Consultant of: Bristol Myers Squibb, Sanofi, VielaBio, Novartis, Marleen Nys Shareholder of: Bristol Myers Squibb, Employee of: Bristol Myers Squibb, Jacques-Eric Gottenberg Grant/research support from: Bristol Myers Squibb, Pfizer, Renaud FELTEN: None declared, Neelanjana Ray Shareholder of: Bristol Myers Squibb, Employee of: Bristol Myers Squibb, Arjan Vissink: None declared, Frans G.M. Kroese Speakers bureau: Bristol Myers Squibb, Roche and Janssen-Cilag, Consultant of: Bristol Myers Squibb, Grant/research support from: Unrestricted grants from Bristol Myers Squibb, Hendrika Bootsma Speakers bureau: Bristol Myers Squibb and Novartis, Consultant of: Bristol Myers Squibb, Roche, Novartis, Medimmune, Union Chimique Belge, Grant/research support from: Unrestricted grants from Bristol Myers Squibb and Roche

Published
2021
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24. Un cas de maladie du pool plaquettaire vide associé à un syndrome de Gougerot-Sjögren primitif

Author

Arnaud Dupuis, Anne-Sophie Korganow, M. Martin, Anita Eckly, Christian Gachet, and R. Felten

Subjects
030203 arthritis & rheumatology, 03 medical and health sciences, 0302 clinical medicine, Gastroenterology, Internal Medicine, 030217 neurology & neurosurgery
Abstract

Introduction La maladie du pool vide plaquettaire (ou Delta-Storage Pool Disease, δ-SPD) est une thrombopathie principalement hereditaire, caracterisee par un deficit quantitatif et/ou qualitatif en granules δ et de leur contenu (adenosine diphosphate (ADP) et serotonine), entrainant des syndromes hemorragiques d’intensite variable. De rares cas de δ-SPD acquis ont ete decrit, principalement associes a des hemopathies ou un lupus erythemateux systemique [1] . Nous rapportons ici le premier cas a notre connaissance de δ-SPD associe a un syndrome de Gougerot-Sjogren primitif (SSp) et reversible sous glucocorticoides et immunoglobulines intraveineuses (IgIV) Observation Une femme de 74 ans a ete hospitalisee pour rupture splenique spontanee. Elle avait beneficie 7 ans auparavant d’un remplacement valvulaire mecanique pour stenose aortique, sans complication, et etait depuis sous anticoagulant oral (fluindione). Depuis 4 ans, elle presentait des episodes hemorragiques survenant hors contexte de surdosage en fluindione ou de thrombopenie. A l’admission, le taux plaquettaire, les temps de prothrombine, de cephaline activee et d’occlusion plaquettaire etaient normaux, de meme que le facteur von Willebrand et l’activite cofacteur de la ristocetine. La recherche d’anticorps anti-plaquettes etait negative. Les tests specifiques ont revele une diminution de l’agregation plaquettaire induite par l’ADP, associee a une faible concentration en ADP et en serotonine plaquettaires, ainsi qu’une reduction de moitie du nombre de granules denses plaquettaire comparativement aux controles, sans aucun signe de deficit en granules alpha ou d’activation plaquettaire. Le diagnostic de δ-SPD avec deficit en ADP a ete retenu. La biopsie osteomedullaire et le scanner thoraco-abdomino-pelvien n’ont pas montre d’arguments pour une hemopathie sous-jacente. L’association d’un syndrome sec occulo-buccal ancien avec test de Shirmer positif, et d’anticorps anti-SSA au 1/1280e antinucleaires positifs a permis d’identifier un SSp associe. Il n’existait aucun passe hemorragique chez les apparentes au 1er et 2e degres et le depistage systematique des anomalies plaquettaires chez les 3 enfants de la patiente est revenu negatif. La mise en contact de plaquettes controle avec du plasma de notre patiente n’a pas apporte d’arguments pour l’hypothese d’une thrombopathie induite par un facteur serique. Devant des episodes hemorragiques spontanes iteratifs et le contexte auto-immun associe, des glucocorticoides probabilistes ont ete instaures (methylprednisolone 500 mg/j durant 3 jours, puis prednisone 1 mg/kg/j avec decroissance lente), suivie par des IgIV (1 g/kg) durant 4 mois. Sous ce traitement, et avec un recul de 36 mois depuis leur arret, la patiente n’a pas presente de recidive hemorragique malgre la poursuite necessaire de la fluindione avec INR cible 2–2,5. Les tests fonctionnels et le dosage de la serotonine plaquettaire ne se sont toutefois normalises que 9 mois et 12 mois apres l’arret des IgIV et de la corticotherapie respectivement, mais restent stables depuis. Discussion La physiopathologie du δ-SPD acquise est inconnue a ce jour. L’activation plaquettaire et endotheliale est augmentee dans les cas d’inflammation et d’activation immunitaire chroniques, tels que le SSp [2] . D’autre part, la serotonine plaquettaire, qui joue un role crucial dans l’agregation, a ete recemment rapportee a des taux plus faibles dans le SSp sans que son role soit clairement defini [3] . Ainsi, il est possible que chez notre patiente, les glucocorticoides et les IgIV aient initialement reduit un etat d’immuno-inflammation au niveau cellulaire et retablit la regulation serotoninergique plaquettaire, expliquant la normalisation plus tardive des tests d’hemostase. La prise en charge du δ-SPD reste actuellement principalement preventive, ou symptomatique par transfusions plaquettaire, desmopressine ou facteur VIIa recombinant en cas de saignement. Conclusion Nous rapportons ici le 1er cas de δ-SPD acquis associe a un SSp et reversible sous glucocorticoides et IvIg et souligne l’importance de savoir evoquer cette pathologie en cas de syndrome hemorragique hors contexte de thrombopenie, de maladie de von Willebrand et des troubles de l’hemostase secondaire.

Published
2018
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25. List of Contributors

Author

A. Alunno, S. Appel, E. Astorri, C. Baldini, F. Barone, E. Bartoloni, M. Bombardieri, S. Bombardieri, S.J. Bowman, J. Campos, F. Carubbi, P. Cipriani, S. Colafrancesco, S. De Vita, N. Del Papa, V. Devauchelle-Pensec, R. Felten, B.A. Fisher, C.M. Fox, R.I. Fox, S. Gandolfo, R. Gerli, R. Giacomelli, J.-E. Gottenberg, R. Jonsson, E.K. Kapsogeorgou, V.C. Kyttaris, D. Lucchesi, C. Lunardi, M.N. Manoussakis, C.P. Mavragani, G. Patuzzo, C. Perricone, J.-O. Pers, C. Pitzalis, R. Priori, L. Quartuccio, Y. Shoenfeld, J. Sibilia, E. Tinazzi, G.C. Tsokos, A.G. Tzioufas, G. Valesini, C. Vitali, and P. Youinou

Published
2016
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26. FUNDAMENTALS FOR INTEGRATION OF SOMATIC HYBRIDIZATION IN ROSE BREEDING

Author

R. Felten, A. Schum, and K. Hofmann

Subjects
Somatic fusion, Rosa wichuraiana, Horticulture, biology, Rosa multiflora, Callus, biology.hybrid_parent_classification, Heterologous, Introgression, Protoplast, biology.organism_classification, Diplocarpon rosae
Abstract

With the intention to exploit new sources of disease resistance in rose breeding, the feasibility of introgression of genes by means of somatic hybridization is evaluated. Protocols have been established for (I) regeneration of protopasts in a variety of rose genotypes, (II) PEG mediated fusion, and (III) preferential regeneration of heterologous fusion products. Protoplasts isolated from non embryogenic source material gave rise to callus in R. canina, R. caudata, R. corymbifera 'Laxa', R. multiflora (two accessions), R. roxburghii, R. spinosissima, R. wichuraiana (two accessions), as well as in R. x hybrida 'Elina' and 'Pariser Charme'. Protoplasts isolated from embryogenic cell suspensions of 'Heckenzauber' and 'Pariser Charme', as well as from non embryogenic suspensions of the hybrid R. persica x R. xanthina were regenerated into plants. In order to suppress sustained cell divisions of non-fused protoplasts or of homologous fusion products, protoplasts were pretreated with either rhodamine 6G (0.1 mmol) or iodoacetate (0.5 – 1 mmol) for 15 minutes as well as with X-rays (300 Gy) at a dose rate of 3 Gy/min. Induced defects are mostly complementary, thus corresponding pretreatment of protoplasts prior to fusion allows preferential regeneration of the heterologous fusion products aimed at. Specific genotypes of different wild species within the genus Rosa were identified to carry resistance genes against Diplocarpon rosae, the causal agent of blackspot (von Malek-Podjaski, 1999). For introgression of resistance into cultivars by means of somatic hybridization, experiments concentrate at the time being on diploid accessions of Rosa multiflora, Rosa wichuraiana and Rosa roxburghii. Putative somatic hybrid callus lines were obtained from 'Heckenzauber' + Rosa wichuraiana or Rosa multiflora as well as from 'Pariser Charme' + Rosa wichuraiana, Rosa multiflora or Rosa roxburghii, respectively. Shoots were regenerated from the combination of 'Pariser Charme' and Rosa wichuraiana. The hybrid character of some selected regenerates was exemplarily confirmed by flow cytometry and AFLP-analysis.

Published
2002
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28. The Significance of Diagnostic Imaging in Acute and Chronic Brain Damage in Boxing

Author

W Funke, R Felten, R Felix, M Holzgraefe, and W Lemme

Subjects
Pathology, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Physical Therapy, Sports Therapy and Rehabilitation, Magnetic resonance imaging, Brain damage, medicine.disease, Hematoma, Chronic Brain Damage, medicine, Medical imaging, Orthopedics and Sports Medicine, Chronic Encephalopathy, medicine.symptom, Prospective cohort study, business, human activities, Amateur
Abstract

The significance and possible extent of structural damage to the central nervous system (CNS) due to boxing are investigated. Bleeding, especially microhematomas, is considered to be one probable cause of the chronic encephalopathy in boxers. In a prospective study, 13 amateur boxers were investigated with the help of MRI several times before and after their fights. The MRI investigations were accompanied by neurologic examinations before and after the fights. Among the 13 boxes, 5 demonstrated focal neurological signs following the fights, without evidence of small hematoma or other structural alterations. The number of head punches did not correlate with the occurrence of neurologic signs. These results indicate that up to now imaging methods cannot clarify the development of chronic encephalopathy.

Published
1992
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29. Prospective evaluation of a stiff shaft glide wire compared with the standard straight wire in crossing severely stenotic aortic valves

Author

William R. Felten, Louis Cannon, John A. Ambrose, Thomas P. Cocke, John Collins, Peter G. Fattal, Douglas Israel, Samin K. Sharma, and George Dangas

Subjects
Aortic valve disease, Aortic valve, medicine.medical_specialty, animal structures, medicine.diagnostic_test, business.industry, musculoskeletal, neural, and ocular physiology, macromolecular substances, Aorta arch, medicine.disease, Prospective evaluation, Valvula aortica, Stenosis, medicine.anatomical_structure, Crossover rate, Internal medicine, medicine, Cardiology, Fluoroscopy, Cardiology and Cardiovascular Medicine, business
Abstract

In this prospective randomized multicenter trial comparing the stiff shaft Terumo glide wire with the conventional fixed-core straight metal guidewire for crossing of severely stenotic aortic valves, the use of the glide wire was the sole correlate of lower mean fluoroscopy time and crossover rate compared with the other technique. These results support the use of the glide wire as the initial wire in crossing severely stenotic aortic valves.

Published
1997
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32. Prospective evaluation of a stiff shaft glide wire compared with the standard straight wire in crossing severely stenotic aortic valves

Author

S K, Sharma, G, Dangas, D, Israel, J, Collins, W R, Felten, P G, Fattal, T P, Cocke, J A, Ambrose, and L, Cannon

Subjects
Male, Titanium, Cardiac Catheterization, Biocompatible Materials, Aortic Valve Stenosis, Equipment Design, Middle Aged, Elasticity, Nickel, Fluoroscopy, Alloys, Humans, Female, Prospective Studies, Aged
Abstract

In this prospective randomized study of the use of the Terumo glide wire compared with the standard straight wire for crossing of severely stenotic aortic valves, the glide wire was shown to significantly decrease the fluoroscopy time of the procedure and to lower by 3.4 times the need for crossover to the alternative technique.

Published
1997

33. The significance of diagnostic imaging in acute and chronic brain damage in boxing. A prospective study in amateur boxing using magnetic resonance imaging (MRI)

Author

M, Holzgraefe, W, Lemme, W, Funke, R, Felix, and R, Felten

Subjects
Adult, Brain Injuries, Acute Disease, Humans, Brain Damage, Chronic, Prospective Studies, Boxing, Magnetic Resonance Imaging, Cerebral Hemorrhage
Abstract

The significance and possible extent of structural damage to the central nervous system (CNS) due to boxing are investigated. Bleeding, especially microhematomas, is considered to be one probable cause of the chronic encephalopathy in boxers. In a prospective study, 13 amateur boxers were investigated with the help of MRI several times before and after their fights. The MRI investigations were accompanied by neurologic examinations before and after the fights. Among the 13 boxes, 5 demonstrated focal neurological signs following the fights, without evidence of small hematoma or other structural alterations. The number of head punches did not correlate with the occurrence of neurologic signs. These results indicate that up to now imaging methods cannot clarify the development of chronic encephalopathy.

Published
1992

34. Low temperature specific heat and electrical resistivity of UCu4.5Al7.5

Author

W. Suski, Frank Steglich, R. Felten, L. Pawlak, M. Drulis, B. Stalínski, and A. Daran

Subjects
Crystal, Field (physics), Specific heat, Condensed matter physics, Electrical resistivity and conductivity, Magnetic order, Chemistry, Heavy fermion, Physical and Theoretical Chemistry, Anomaly (physics), Condensed Matter Physics, Instrumentation
Abstract

The specific heat and electrical resistivity results are presented for UCu 4.5 Al 7.5 , a magnetically ordered nearly heavy fermion compound. The specific heat data do not indicate the expected anomaly characteristic for the magnetic order transition; only a very weak one was detected, which has been separated using a simple theoretical procedure. The electronic specific heat coefficient has been estimated to be 118 mJ mol −1 K −2 . The other heavy fermion coefficients have also been calculated. The electrical resistivity data for UCu 4.5 Al 7.5 include indications of strong crystal field effects.

Published
1989
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35. Crystal-field effects and f-derived specific heats in heavy-fermion compounds

Author

B. Renker, R. Felten, H. Rietschel, Frank Steglich, and G. Weber

Subjects
Crystal, Materials science, Field (physics), Heavy fermion, Extraction (chemistry), Thermodynamics, Calorimetry, Atmospheric temperature range, Condensed Matter Physics, Ground state, Electron localization function, Electronic, Optical and Magnetic Materials
Abstract

We discuss experimetal results of calorimetry on heavy-fermion compounds (HFC) with special regard to the f-derived specific heat ΔC . Attention is given to the extraction of Δ C and the uncertainties implied therein. The discussion includes some Ce-based 4f systems but concentrates on U-based 5f HFC. In four of these (UBe 13 , UPt 3 , URu 2 Si 2 , U 2 Zn 17 ) distinct anomalies in Δ C have recently been found in the temperature range between 20 and 100 K which we think are likely to be caused by crystal-field effects thus indicating strong 5f localization.

Published
1988
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36. Normal ground-state properties of heavy-fermion actinide compounds

Author

E. Gering, B. Renker, Frank Steglich, P. Frings, F. Gompf, G. Weber, H. Rietschel, and R. Felten

Subjects
Physics, Lattice dynamics, Superconductivity, Condensed matter physics, High Energy Physics::Lattice, General Engineering, Electronic structure, Actinide, Resonance (particle physics), Condensed Matter::Superconductivity, Heavy fermion, Condensed Matter::Strongly Correlated Electrons, Kondo effect, Nuclear Experiment, Ground state
Abstract

We present experimental results for the lattice dynamics in UPt3 and for the electronic specific heat in UPt3 and URu2Si2, which, together with already published similar results for UBe13, indicate that for the actinide-based heavy-fermion superconductors, the normal ground-state is that of localized 5f-electrons and the heavy-fermion properties are due to a low-T Kondo resonance.

Published
1987
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37. Observation of a Schottky Anomaly in the Specific Heat of the Heavy-Fermion Compound UBe 13

Author

H. Rietschel, R. Felten, F. Gompf, B. Renker, Frank Steglich, J. Beuers, and G. Weber

Subjects
Materials science, Condensed matter physics, Specific heat, Extraction (chemistry), Intermetallic, General Physics and Astronomy, Calorimetry, Electron, Atmospheric temperature range, Schottky anomaly, Inelastic neutron scattering
Abstract

We present the results of calorimetric measurements of the specific heat in UBe13 and ThBe13 in the temperature range 20 K T 120 K. Combined with earlier results of inelastic neutron scattering, the data allow the extraction of the electronic specific heat ΔC in UBe13. ΔC shows a pronounced peak around 70 K which we interpret as a Schottky anomaly due to crystal-field splitting of a 5f3 ground-state configuration. Our results suggest the existence of highly localized 5f electrons in the heavy-fermion compound UBe13.

Published
1986
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38. Magnetization and specific heat of CeAl3

Author

C. D. Bredl, Frank Steglich, W. Lieke, U. Rauchschwalbe, G. Weber, R. Felten, U. Umhofer, J.C.P. Klaasse, Jan Aarts, and F.R. de Boer

Subjects
Magnetization, Materials science, Specific heat, Condensed matter physics, Binary alloy, Intermetallic, Kondo effect, Condensed Matter Physics, Wilson ratio, Magnetic susceptibility, Electronic, Optical and Magnetic Materials, Magnetic field
Abstract

Measurements of the high-field dc magnetization and low-field ac susceptibility as well as specific-heat experiments covering almost four decades in temperature characterize CeAl 3 as a “dense Kondo system” with T k ≈ 5 K. From these results, the low-temperature value of the “Wilson ratio”, R (0) = 2.9, is deduced.

Published
1985
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39. An inelastic neutron scattering study on the heavy fermion systems CeCu 2 Ge 2 and CeAg 2 Ge 2

Author

Alois Loidl, U. Rauchschwalbe, K. Knorr, G. Knopp, A. P. Murani, R. Felten, Frank Steglich, G. Weber, and H. Spille

Subjects
Physics, Quasielastic scattering, Condensed matter physics, Dynamic structure factor, Neutron scattering, Inelastic scattering, Condensed Matter Physics, Deep inelastic scattering, Small-angle neutron scattering, Inelastic neutron scattering, Electronic, Optical and Magnetic Materials, Nuclear physics, Quasielastic neutron scattering, Nuclear Experiment
Abstract

An inelastic neutron scattering study is performed on the new magnetically ordered heavy-fermion systems CeCu2Ge2 and CeAg2Ge2. The temperature dependence of the quasielastic line can be interpreted in terms of a Kondo type of behavior. In addition crystalline electric field transition energies are reported.

Published
1987
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40. Defect contribution to the high temperature specific heat of polycrystalline CeCu2Si2

Author

G. Weber, R. Felten, U. Umhofer, and U. Rauchschwalbe

Subjects
Materials science, Specific heat, Thermodynamics, Activation energy, Crystallite, Condensed Matter Physics, Electronic, Optical and Magnetic Materials
Abstract

The specific heat of polycrystalline CeCu 2 Si 2 has been measured between 20 and 400 K and shows a contribution, which is tentatively ascribed to Schottky-defects with an activation energy of k B 1600 K. These defects might be the cause for the irregularities observed in CeCu 2 Si 2 at low temperature.

Published
1985
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41. Transition from Kondo to intermediate valence in Ce1−xYxAl2

Author

R. Felten, J. Heibel, R. Schefzyk, Frank Steglich, and G. Weber

Subjects
Valence (chemistry), Materials science, Specific heat, Condensed matter physics, Continuous transition, Kondo insulator, Kondo effect, Condensed Matter Physics, Electronic, Optical and Magnetic Materials
Abstract

High-temperature specific heat measurements and an extensive study of the thermal-expansion coefficient on Ce 1− x Y x Al 2 reveal for x ⩽ 0.6 trivalent Ce-ions, which are subject to Kondo and crystal-field effects. A continuous transition into an intermediate valent state occurs for higher Y concentrations.

Published
1985
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42. Specific heats and crystal-field splittings of CeCu 2 Ge 2 , CeRu 2 Ge 2 and UBe 13

Author

H. Rietschel, G. Weber, and R. Felten

Subjects
Materials science, Specific heat, Condensed matter physics, Ferromagnetism, Crystal field theory, Magnetic order, Schottky defect, Intermetallic, Antiferromagnetism, Schottky diode, Condensed Matter Physics, Electronic, Optical and Magnetic Materials
Abstract

The f-electron contributions to the specific heats of CeCu2Ge2, CeRu2Ge2 and UBe13 were determined and show Schottky anomalies at temperatures between 50 and 250 K. From these the crystal-field splittings are deduced. The specific heat connected with the magnetic phase transition in CeRu2.16Ge2 was measured and a second anomaly observed, which points to a complicated magnetic order.

Published
1987
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43. Specific heat and thermal expansion of CeCu2Si2 at low temperature

Author

Frank Steglich, R. Schefzyk, J.C.P. Klaasse, Jan Aarts, Michael Lang, F.R. de Boer, G. Weber, W. Lieke, C. D. Bredl, S. Riegel, R. Felten, and U. Rauchschwalbe

Subjects
Superconductivity, Reduction (complexity), Materials science, Volume (thermodynamics), Condensed matter physics, Specific heat, Thermodynamics, equipment and supplies, Condensed Matter Physics, Stoichiometry, Thermal expansion, Electronic, Optical and Magnetic Materials
Abstract

Specific-heat and thermal-expansion measurements on CeCu2Si2 samples of varying stoichiometry as well as on dilute (Ce, T)Cu2Si2 alloys (T:Y,La) indicate that the observed suppression of superconductivity in samples with “high” unit-cell volume is associated with a reduction of the Kondo temperature and the occurrence of another cooperative phenomenon, probably magnetic in origin.

Published
1985
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47. Infrared detector arrays with multiplexing cryogenic read-out electronics for isophot

Author

R. Felten, R. Faymonville, D. Engemann, A. Sohn, J. Vermeiren, B. Dierickx, K. Meyer, and O. Frenzl

Subjects
Physics, Infrared astronomy, business.industry, Infrared, Detector, General Engineering, Multiplexing, Responsivity, Optics, CMOS, Optoelectronics, Infrared detector, business, Electronic circuit
Abstract

Cryogenic Read out Electronic circuits (CRE) are developed in a CMOS technology for the multiplexing operation at temperatures around 4 K and below of extrinsic photoconducting detectors and detector arrays of Ge and Si in the Infrared Space Observatory (ISO) instrument ISOPHOT covering a wavelength region between 10–200 μm. Measurements on the 66 elements spectroscopic array ISOPHOTS2 show performance data of an NEP around 4 × 10−17W/√Hz and a voltage responsivity of 1014V/Ws at low background operation.

48. Unmet needs in axial spondyloarthritis. Proceedings of the French spondyloarthritis taskforce workshop.

Author

Wendling D, Breban M, Costantino F, Lequerré T, Felten R, Ruyssen-Witrand A, Tournadre A, Vegas LP, Marotte H, Baillet A, Loeuille D, Lukas C, Miceli-Richard C, Gossec L, Molto A, Goupille P, Pham T, Dernis E, Claudepierre P, Verhoeven F, and Prati C

Subjects
Humans, France, Female, Advisory Committees, Male, Biomarkers, Spondylarthritis diagnosis, Spondylarthritis therapy, Axial Spondyloarthritis diagnosis, Axial Spondyloarthritis therapy
Abstract

The progress observed over the last 30 years in the field of axial spondyloarthritis (axSpA) has not made it possible to answer all the current questions. This manuscript represents the proceedings of the meeting of the French spondyloArthitiS Task force (FAST) in Besançon on September 28 and 29, 2023. Different points of discussion were thus individualized as unmet needs: biomarkers for early diagnosis and disease activity, a common electronic file dedicated to SpA nationwide, a better comprehension of dysbiosis in the disease, a check-list for addressing to the rheumatologist, adapt patient reported outcomes thresholds for female gender, implementation of comorbidities screening programs, new imaging tools, in research cellular and multi omics approaches, grouping, at a nationwide level, different cohorts and registries, therapeutic strategy studies, consensual definition of difficult to treat disease and management, preclinical stage of the disease, mastering AI as a tool in the various aspects of research. These elements may represent a framework for the research agenda in axSpA for the years to come., (Copyright © 2024 The Author(s). Published by Elsevier Masson SAS.. All rights reserved.)

Published
2024
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49. IL-17 inhibitors in axial spondyloarthritis. An overview.

Author

Toussirot E and Felten R

Subjects
Humans, Disease Progression, Antirheumatic Agents therapeutic use, Animals, Interleukin-17 antagonists & inhibitors, Interleukin-17 immunology, Axial Spondyloarthritis drug therapy
Abstract

Introduction: The therapeutic armamentarium for spondyloarthritis has expanded considerably in recent years, and there is growing evidence to support the increasing use of IL-17 inhibitors (IL-17i) in axial spondyloarthritis (axSpA)., Areas Covered: This literature review provides an update on the role of IL-17 in the pathogenesis of axSpA, efficacy and safety from clinical trials and real-life studies on the use of IL17i in axSpA. We also review the impact of extra-musculoskeletal manifestations on the decision to treat with IL17i and the efficacy of IL17i on structural progression., Expert Opinion: There are still some unanswered questions concerning the use of IL-17i in axSpA in clinical practice such as their respective place in the management of axSpA compared to TNFα inhibitors (TNFi). Their main differences rely on their specific efficacy in extra-articular manifestations such as psoriasis, uveitis, and inflammatory bowel diseases leading to the choice of the best treatment in a given patient. Regarding their real impact on structural progression, the rate of progression under IL-17i appears to be low and presumably similar to TNFi. One final question is the advantage of blocking the two IL-17 isoforms A and F compared to the single inhibition of IL-17A.

Published
2024
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50. Efficacy of BAFF inhibition and B-cell depletion in non-obese diabetic mice as a spontaneous model for Sjögren's disease.

Author

Felten R, Foray AP, Schneider P, Marquet C, Pecquet C, Monneaux F, Dumortier H, Sibilia J, Valette F, Chatenoud L, and Gottenberg JE

Subjects
Animals, Mice, Female, Salivary Glands pathology, Salivary Glands metabolism, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal pharmacology, Lymphocyte Depletion, B-Cell Activating Factor antagonists & inhibitors, B-Cell Activating Factor metabolism, Sjogren's Syndrome immunology, Mice, Inbred NOD, Disease Models, Animal, B-Lymphocytes immunology, B-Lymphocytes metabolism
Abstract

Introduction: The therapeutic interest of targeting B-cell activating factor (BAFF) in Sjögren's disease (SjD) can be suspected from the results of two phase II clinical trials but has not been evaluated in an animal model of the disease. We aimed to evaluate the therapeutic efficacy of this strategy on dryness and salivary gland (SG) infiltrates in the NOD mouse model of SjD., Material and Methods: Female NOD mice between ages 10 and 18 weeks were treated with a BAFF-blocking monoclonal antibody, Sandy-2 or an isotype control. Dryness was measured by the stimulated salivary flow. Salivary lymphocytic infiltrates were assessed by immunohistochemistry. Blood, SGs, spleen and lymph-node lymphocyte subpopulations were analysed by flow cytometry. SG mRNA expression was analysed by transcriptomic analysis., Results: BAFF inhibition significantly decreased SG lymphocytic infiltrates, which was inversely correlated with salivary flow. The treatment markedly decreased B-cell number in SGs, blood, lymph nodes and spleen and increased Foxp3 + regulatory and CD3 + CD4 - CD8 - double negative T-cell numbers in SGs., Conclusion: A monoclonal antibody blocking BAFF and depleting B cells had therapeutic effectiveness in the NOD mouse model of SjD. The increase in regulatory T-lymphocyte populations might underlie the efficacy of this treatment., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2024
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