Your search keyword '"Diot E"' showing total 12 results

1. Evidence of the contribution of the X chromosome to systemic sclerosis susceptibility: Association with the functional IRAK1 196Phe/532Ser haplotype

Author

Dieude, P., Bouaziz, M., Guedj, M., Riemekasten, G., Airo, P., Mueller, M., Cusi, D., Matucci-Cerinic, M., Melchers, I., Koenig, W., Salvi, E., Wichmann, H. E., Cuomo, G., Hachulla, E., Diot, E., Hunzelmann, N., Caramaschi, P., Mouthon, L., Riccieri, V., Distler, J., Tarner, I., Avouac, J., Meyer, O., Kahan, A., Chiocchia, G., Boileau, C., Allanore, Y., Dieude, P., Bouaziz, M., Guedj, M., Riemekasten, G., Airo, P., Mueller, M., Cusi, D., Matucci-Cerinic, M., Melchers, I., Koenig, W., Salvi, E., Wichmann, H. E., Cuomo, G., Hachulla, E., Diot, E., Hunzelmann, N., Caramaschi, P., Mouthon, L., Riccieri, V., Distler, J., Tarner, I., Avouac, J., Meyer, O., Kahan, A., Chiocchia, G., Boileau, C., and Allanore, Y.

Abstract

Objective Several autoimmune disorders, including systemic sclerosis (SSc), are characterized by a strong sex bias. To date, it is not known whether genes on the sex chromosomes influence SSc susceptibility. Recently, an IRAK1 haplotype that contains the 196Phe functional variant (rs1059702), located on Xq28, was found to confer susceptibility to systemic lupus erythematosus (SLE). This study was undertaken to test for an association between SSc and the IRAK1 SLE risk haplotype. Methods. We tested for an association with the IRAK1 SLE risk haplotype in a discovery set of 849 SSc patients and 625 controls. IRAK1 rs1059702 was further genotyped in a replication set, which included Caucasian women from Italy (493 SSc patients and 509 controls) and Germany (466 SSc patients and 1,083 controls). Results. An association between the IRAK1 haplotype and SSc was detected in the discovery set. In both the discovery and replication sets, the rs1059702 TT genotype was found to be associated with specific SSc subsets, highlighting a potential contribution to disease severity. A meta-analysis provided evidence of an association of both the T allele and TT genotype with the overall disease, with an odds ratio (OR) of 1.20 and 95% confidence interval (95% CI) of 1.06- 1.35 for the T allele (P = 0.003) and an OR of 1.49 and 95% CI of 1.06- 2.10 for the TT genotype (P = 0.023). However, the most notable associations were observed with the diffuse cutaneous, anti- topoisomerase I antibody positive, and SSc-related fibrosing alveolitis subsets (OR 2.35 [95% CI 1.51- 3.66], P = 1.56 x 10(-4), OR 2.84 [95% CI 1.87- 4.32], P = 1.07 x 10(-6), and OR 2.09 [95% CI 1.35- 3.24], P = 9.05 x 10(-4), respectively). Conclusion. Our study provides the first evidence of an association between IRAK1 and SSc, demonstrating that a sex chromosome gene directly influences SSc susceptibility and its phenotypic heterogeneity.

Published

2011

2. Association of a KCNA5 Gene Polymorphism With Systemic Sclerosis-Associated Pulmonary Arterial Hypertension in the European Caucasian Population

Author

Wipff, J., Dieude, P., Guedj, M., Ruiz, B., Riemekasten, G., Cracowski, J. L., Matucci-Cerinic, M., Melchers, I., Humbert, M., Hachulla, E., Airo, P., Diot, E., Hunzelmann, N., Caramaschi, P., Sibilia, J., Valentini, G., Tiev, K., Girerd, B., Mouthon, L., Riccieri, V., Carpentier, P. H., Distler, J., Amoura, Z., Tarner, I., Degano, B., Avouac, J., Meyer, O., Kahan, A., Boileau, C., Allanore, Y., Wipff, J., Dieude, P., Guedj, M., Ruiz, B., Riemekasten, G., Cracowski, J. L., Matucci-Cerinic, M., Melchers, I., Humbert, M., Hachulla, E., Airo, P., Diot, E., Hunzelmann, N., Caramaschi, P., Sibilia, J., Valentini, G., Tiev, K., Girerd, B., Mouthon, L., Riccieri, V., Carpentier, P. H., Distler, J., Amoura, Z., Tarner, I., Degano, B., Avouac, J., Meyer, O., Kahan, A., Boileau, C., and Allanore, Y.

Abstract

Objective. Pulmonary arterial hypertension (PAH) has emerged as a leading cause of death in systemic sclerosis (SSc). The genetic basis of PAH has been unraveled in recent years, with a major role played by transforming growth factor beta receptors; however, some other candidate genes have also been advocated, including potassium voltage-gated channel, shaker-related subfamily, member 5 (KCNA5). We undertook this study to determine whether KCNA5 polymorphisms confer susceptibility to SSc and its vascular phenotype, including PAH. Methods. Four KCNA5 single-nucleotide polymorphisms (SNPs), rs10744676, rs1860420, rs3741930, and rs2284136, were genotyped in a discovery set of 638 SSc patients and 469 controls. In addition, rs10744676 was genotyped in an independent replication sample (938 SSc patients and 564 controls) and in a cohort of 168 patients with different PAH subtypes. Results. The KCNA5 rs10744676 variant was found to be associated with SSc in the discovery sample, with an odds ratio (OR) of 0.62 (95% confidence interval [95% CI] 0.48-0.79, adjusted P = 0.0003) in comparison with controls (C allele frequency 11.4% versus 17.2%). When subphenotypes were investigated, an association was found solely for PAH associated with SSc (OR 0.31 [95% CI 0.13-0.71], adjusted P = 0.04). The other KCNA5 SNPs tested were not associated with any SSc subset. The above association with PAH associated with SSc was replicated in the second set. In the combined population, rs10744676 was strongly associated with PAH associated with SSc in comparison with controls (OR 0.36 [95% CI 0.21-0.63], P = 0.0002). In the independent cohort of patients with PAH, after investigating PAH subtypes, only rs10744676 showed an association with PAH associated with SSc. Conclusion. Our results provide the first evidence for an association between the KCNA5 rs10744676 variant and PAH associated with SSc.

Published

2010

3. Evidence of the contribution of the X chromosome to systemic sclerosis susceptibility: Association with the functional IRAK1 196Phe/532Ser haplotype

Author

Dieudé, P., primary, Bouaziz, M., additional, Guedj, M., additional, Riemekasten, G., additional, Airò, P., additional, Müller, M., additional, Cusi, D., additional, Matucci-Cerinic, M., additional, Melchers, I., additional, Koenig, W., additional, Salvi, E., additional, Wichmann, H. E., additional, Cuomo, G., additional, Hachulla, E., additional, Diot, E., additional, Hunzelmann, N., additional, Caramaschi, P., additional, Mouthon, L., additional, Riccieri, V., additional, Distler, J., additional, Tarner, I., additional, Avouac, J., additional, Meyer, O., additional, Kahan, A., additional, Chiocchia, G., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2011

4. Association of the CD226 Ser307 variant with systemic sclerosis: Evidence of a contribution of costimulation pathways in systemic sclerosis pathogenesis

Author

Dieudé, P., primary, Guedj, M., additional, Truchetet, M. E., additional, Wipff, J., additional, Revillod, L., additional, Riemekasten, G., additional, Matucci-Cerinic, M., additional, Melchers, I., additional, Hachulla, E., additional, Airo, P., additional, Diot, E., additional, Hunzelmann, N., additional, Mouthon, L., additional, Cabane, J., additional, Cracowski, J. L., additional, Riccieri, V., additional, Distler, J., additional, Amoura, Z., additional, Valentini, G., additional, Camaraschi, P., additional, Tarner, I., additional, Frances, C., additional, Carpentier, P., additional, Brembilla, N. C., additional, Meyer, O., additional, Kahan, A., additional, Chizzolini, C., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2011

5. Association of a KCNA5 gene polymorphism with systemic sclerosis–associated pulmonary arterial hypertension in the European Caucasian population

Author

Wipff, J., primary, Dieudé, P., additional, Guedj, M., additional, Ruiz, B., additional, Riemekasten, G., additional, Cracowski, J. L., additional, Matucci‐Cerinic, M., additional, Melchers, I., additional, Humbert, M., additional, Hachulla, E., additional, Airo, P., additional, Diot, E., additional, Hunzelmann, N., additional, Caramaschi, P., additional, Sibilia, J., additional, Valentini, G., additional, Tiev, K., additional, Girerd, B., additional, Mouthon, L., additional, Riccieri, V., additional, Carpentier, P. H., additional, Distler, J., additional, Amoura, Z., additional, Tarner, I., additional, Degano, B., additional, Avouac, J., additional, Meyer, O., additional, Kahan, A., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2010

6. BANK1 is a genetic risk factor for diffuse cutaneous systemic sclerosis and has additive effects with IRF5 and STAT4

Author

Dieudé, P., primary, Wipff, J., additional, Guedj, M., additional, Ruiz, B., additional, Melchers, I., additional, Hachulla, E., additional, Riemekasten, G., additional, Diot, E., additional, Hunzelmann, N., additional, Sibilia, J., additional, Tiev, K., additional, Mouthon, L., additional, Cracowski, J. L., additional, Carpentier, P. H., additional, Distler, J., additional, Amoura, Z., additional, Tarner, I., additional, Avouac, J., additional, Meyer, O., additional, Kahan, A., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2009

7. STAT4 is a genetic risk factor for systemic sclerosis having additive effects with IRF5 on disease susceptibility and related pulmonary fibrosis

Author

Dieudé, P., primary, Guedj, M., additional, Wipff, J., additional, Ruiz, B., additional, Hachulla, E., additional, Diot, E., additional, Granel, B., additional, Sibilia, J., additional, Tiev, K., additional, Mouthon, L., additional, Cracowski, J.L., additional, Carpentier, P.H., additional, Amoura, Z., additional, Fajardy, I., additional, Avouac, J., additional, Meyer, O., additional, Kahan, A., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2009

8. Association between the IRF5 rs2004640 functional polymorphism and systemic sclerosis: A new perspective for pulmonary fibrosis

Author

Dieudé, P., primary, Guedj, M., additional, Wipff, J., additional, Avouac, J., additional, Fajardy, I., additional, Diot, E., additional, Granel, B., additional, Sibilia, J., additional, Cabane, J., additional, Mouthon, L., additional, Cracowski, J. L., additional, Carpentier, P. H., additional, Hachulla, E., additional, Meyer, O., additional, Kahan, A., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2008

9. ThePTPN22620W allele confers susceptibility to systemic sclerosis: Findings of a large case–control study of European Caucasians and a meta‐analysis

Author

Dieudé, P., primary, Guedj, M., additional, Wipff, J., additional, Avouac, J., additional, Hachulla, E., additional, Diot, E., additional, Granel, B., additional, Sibilia, J., additional, Cabane, J., additional, Meyer, O., additional, Mouthon, L., additional, Kahan, A., additional, Boileau, C., additional, and Allanore, Y., additional

Published

2008

10. Efficacy and Safety of Botulinum Toxin in Adults with Raynaud's Phenomenon Secondary to Systemic Sclerosis: A Multicenter, Randomized, Double-Blind, Placebo-Controlled Study.

Author

Senet P, Maillard H, Diot E, Lazareth I, Blaise S, Arnault JP, Pistorius MA, Boulon C, Cogrel O, Warzocha U, Rivière S, Malloizel-Delaunay J, Servettaz A, Sassolas B, Viguier M, Monfort JB, Janique S, and Vicaut E

Subjects

Humans, Adult, Quality of Life, Hand, Scleroderma, Systemic complications, Scleroderma, Systemic drug therapy, Botulinum Toxins, Type A therapeutic use, Raynaud Disease drug therapy, Raynaud Disease etiology

Abstract

Objective: To determine whether a single session of botulinum toxin type A (BTA) injections into both hands more effectively decreases the frequency of systemic sclerosis-associated Raynaud's phenomenon (SSc-RP) episodes than placebo., Methods: This multicenter, randomized, double-blind, placebo-controlled, parallel-group phase III trial in patients with SSc-RP assessed the effect of 50-unit BTA or placebo injections into the palms of both hands around each neurovascular bundle during 1 session in winter. The primary end point was the between-group difference in the median change in the number of RP episodes from baseline (day 0) to 4 weeks postinjection. Values between the groups were compared with the Wilcoxon rank-sum test., Results: The intent-to-treat analysis included 46 BTA-treated patients and 44 placebo recipients. At 4 weeks after assigned treatment injections, the median number of daily RP episodes decreased comparably in the BTA and placebo groups (median change -1 episode/day [interquartile range (IQR) -1.5, 0 episodes/day] and -1 episode/day [IQR -2.5, 0 episodes/day], respectively) (P = 0.77 versus placebo). Moreover, change in Raynaud's Condition Score, quality of life assessed by Health Assessment Questionnaire disability index, and hand function assessed by shortened Disabilities of the Arm, Shoulder, and Hand (QuickDASH) and Cochin Hand Function Scale from baseline to follow-up weeks 4, 12, and 24 did not differ significantly between groups. The BTA group experienced transient hand muscle weakness significantly more frequently (P = 0.003)., Conclusion: Neither the primary nor secondary end points were reached, and our results do not support any beneficial effect of palmar BTA injections to treat SSc-RP., (© 2022 American College of Rheumatology.)

Published

2023

11. Adding Azathioprine to Remission-Induction Glucocorticoids for Eosinophilic Granulomatosis With Polyangiitis (Churg-Strauss), Microscopic Polyangiitis, or Polyarteritis Nodosa Without Poor Prognosis Factors: A Randomized, Controlled Trial.

Author

Puéchal X, Pagnoux C, Baron G, Quémeneur T, Néel A, Agard C, Lifermann F, Liozon E, Ruivard M, Godmer P, Limal N, Mékinian A, Papo T, Ruppert AM, Bourgarit A, Bienvenu B, Geffray L, Saraux JL, Diot E, Crestani B, Delbrel X, Sailler L, Cohen P, Le Guern V, Terrier B, Groh M, Le Jeunne C, Mouthon L, Ravaud P, and Guillevin L

Subjects

Adult, Aged, Asthma chemically induced, Disease Progression, Double-Blind Method, Drug Therapy, Combination, Female, Humans, Male, Middle Aged, Recurrence, Remission Induction, Rhinitis chemically induced, Sinusitis chemically induced, Azathioprine therapeutic use, Churg-Strauss Syndrome drug therapy, Glucocorticoids therapeutic use, Immunosuppressive Agents therapeutic use, Microscopic Polyangiitis drug therapy, Polyarteritis Nodosa drug therapy

Abstract

Objective: In most patients with nonsevere systemic necrotizing vasculitides (SNVs), remission is achieved with glucocorticoids alone, but one-third experience a relapse within 2 years. This study was undertaken to determine whether the addition of azathioprine (AZA) to glucocorticoids could achieve a higher sustained remission rate of newly diagnosed nonsevere eosinophilic granulomatosis with polyangiitis (Churg-Strauss) (EGPA), microscopic polyangiitis (MPA), or polyarteritis nodosa (PAN)., Methods: All patients included in this double-blind trial received glucocorticoids, gradually tapered over 12 months, and were randomized to receive AZA or placebo for 12 months, with stratification according to SNV (EGPA or MPA/PAN). The primary end point was the combined rate of remission induction failures and minor or major relapses at month 24., Results: Ninety-five patients (51 with EGPA, 25 with MPA, and 19 with PAN) met the inclusion criteria, were randomized, and received at least 1 dose of AZA (n = 46) or placebo (n = 49). At month 24, 47.8% of the patients receiving AZA versus 49% of the patients receiving placebo had remission induction failures or relapses (P = 0.86). Secondary end points were comparable between the AZA and placebo arms. These included initial remission rate (95.7% versus 87.8%), total relapse rate (44.2% versus 40.5%), and glucocorticoid use. Two patients in the placebo arm died; 22 patients in the AZA arm (47.8%) and 23 patients in the placebo arm (46.9%) experienced ≥1 severe adverse event. For EGPA patients, the primary end point (48% in the AZA arm versus 46.2% in the placebo arm) and the percent of patients who experienced asthma/rhinosinusitis exacerbations (24% in the AZA arm versus 19.2% in the placebo arm) were comparable between treatment arms., Conclusion: Addition of AZA to glucocorticoids for the induction of remission of nonsevere SNVs does not improve remission rates, lower relapse risk, spare steroids, or diminish the EGPA asthma/rhinosinusitis exacerbation rate., (© 2017, American College of Rheumatology.)

Published

2017

12. Treatment of systemic necrotizing vasculitides in patients aged sixty-five years or older: results of a multicenter, open-label, randomized controlled trial of corticosteroid and cyclophosphamide-based induction therapy.

Author

Pagnoux C, Quéméneur T, Ninet J, Diot E, Kyndt X, de Wazières B, Reny JL, Puéchal X, le Berruyer PY, Lidove O, Vanhille P, Godmer P, Fain O, Blockmans D, Bienvenu B, Rollot F, Aït el Ghaz-Poignant S, Mahr A, Cohen P, Mouthon L, Perrodeau E, Ravaud P, and Guillevin L

Subjects

Aged, Aged, 80 and over, Azathioprine therapeutic use, Drug Administration Schedule, Drug Therapy, Combination, Female, Humans, Male, Methotrexate therapeutic use, Treatment Outcome, Adrenal Cortex Hormones therapeutic use, Cyclophosphamide therapeutic use, Remission Induction methods, Systemic Vasculitis drug therapy

Abstract

Objective: To investigate a new therapeutic strategy, with rapid corticosteroid dose tapering and limited cyclophosphamide (CYC) exposure, for older patients with systemic necrotizing vasculitides (SNVs; polyarteritis nodosa [PAN], granulomatosis with polyangiitis [Wegnener's] [GPA], microscopic polyangiitis [MPA], or eosinophilic GPA [Churg-Strauss] [EGPA])., Methods: A multicenter, open-label, randomized controlled trial comprising patients ≥65 years old and newly diagnosed as having SNV was conducted. The experimental treatment consisted of corticosteroids for ∼9 months and a maximum of six 500-mg fixed-dose intravenous (IV) CYC pulses, every 2-3 weeks, then maintenance azathioprine or methotrexate. The control treatment included ∼26 months of corticosteroids for all patients, combined with 500 mg/m(2) IV CYC pulses, every 2-3 weeks until remission, then maintenance for all patients with GPA or MPA and for those with EGPA or PAN with a Five-Factors Score (FFS) of ≥1. Randomization used a 1:1 ratio computer-generated list and was performed centrally with sealed opaque envelopes. The primary outcome measure was ≥1 serious adverse event (SAE) occurring within 3 years of followup. Secondary outcome measures included remission and relapse rates., Results: Among the 108 patients randomized, 4 were excluded (early consent withdrawal or protocol violation). Mean ± SD age at diagnosis was 75.2 ± 6.3 years. Analysis at 3 years included 53 patients (21 GPA, 21 MPA, 8 EGPA, and 3 PAN) in the experimental arm and 51 patients (15 GPA, 23 MPA, 6 EGPA, and 7 PAN) in the conventional arm. In total, 32 (60%) versus 40 (78%) had ≥1 SAE (P = 0.04), most frequently infections; 6 (11%) versus 7 (14%) failed to achieve remission (P = 0.71); 9 (17%) versus 12 (24%) died (P = 0.41); and 20 (44%) of 45 versus 12 (29%) of 41 survivors in remission experienced a relapse (P = 0.15)., Conclusion: For older SNV patients, an induction regimen limiting corticosteroid exposure and with fixed low-dose IV CYC pulses reduces SAEs in comparison to conventional therapy, and does not affect the remission rate. Three-year relapse rates remain high for both arms., (Copyright © 2015 by the American College of Rheumatology.)

Published

2015