📇 Rhumatologue · LA ROCHE SUR YON · (85) · Salarié

MME JULIE FLAMENT

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4 lieux d'exercice — choisissez celui qui vous arrange
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97.1 rhumatos / 100 000 hab. — département bien doté

Rhumatologue

📍 LA ROCHE SUR YON (85)SalariéRPPS 10100469724

📊 Reconnaissance scientifique : 7/100📝 22 articles publiés

✨ Génération du profil synthétique IA en cours…

Activité de recherche & publications

Indicateurs publics agrégés sur 250 M+ d'œuvres scientifiques (OpenAlex, PubMed). Traduits ici en langage patient.

Influence scientifique

7 articles ont été cités au moins 7fois par d'autres chercheurs — preuve que ses travaux sont repris par la communauté médicale.

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Données ANS publiques (Licence Ouverte 2.0) · Enrichissements MonRhumato 100 % opt-in · Toute personne référencée peut demander la suppression ou la rectification.

Top publications · les plus citées

Linkage to 18qter differentiates two clinically overlapping syndromes: congenital cataracts-facial dysmorphism-neuropathy (CCFDN) syndrome and Marinesco-Sjögren syndrome

Journal of medical genetics · 2002

📚 20 citations🔓 Open Access📄 PDF gratuit ↗

Soluble HLA-DR antigen levels in serum correlate with rheumatoid arthritis disease activity and the presence of disease-associated epitopes

Tissue antigens · 2000

📚 18 citations

Lire l'abstract Crossref ↓

Acknowledgments:This study was supported by a grant from the Belgian Red Cross. The authors thank Prof. W. Duquet for valuable help with the statistical analysis of the results.Abstract:We investigated correlations between soluble HLA‐DR (sHLA‐DR) molecules and several clinical, biological and genetic parameters associated with rheumatoid arthritis (RA) disease activity. Serum sHLA‐DR concentrations were determined in 146 samples from 89 RA patients by an ELISA format, using an antibody combination of mouse and rat monoclonal anti‐human HLA‐DR antibodies. The mean sHLA‐DR serum level in RA patients was significantly increased with 277±19 ng/ml compared to 142±13 ng/ml of 80 healthy controls (P<0.001). In ascending order of significance, correlations were found between serum sHLA‐DR and EULAR swelling and pain scores, Waaler‐Rose, RA factor, ESR and CRP (P=0.025 to P<0.001). High sHLA‐DR levels were defined above 374 ng/ml that was the 95% confidence interval of the controls. Thirty‐seven blood samples (25%) in 31 RA patients were above this level. The EULAR pain and swelling scores, erythrocyte sedimentation rate (ESR), C‐reactive protein (CRP) and RA factor were higher (P=0.044 to P<0.001) at the moment of high sHLA‐DR concentrations, compared to the lower concentrations. Higher disease activity was further found in groups of RA patients respectively heterozygous or homozygous for the disease‐associated epitope (Q)R/KRAA within the HLA‐DRB1 chain, compared to the group without this epitope (P<0.017 for part of the results). Likewise, sHLA‐DR was respectively 169±17 (no disease associated epitope), 324±34 (heterozygous) and 442±69 ng/ml (homozygous for the disease‐associated epitope on HLA‐DRB1 alleles) (P<0.017). In conclusion, this study shows significant correlations between serum sHLA‐DR levels and RA disease activity parameters, as well as increased sHLA‐DR in patients with disease‐associated epitope on HLA‐DRB1 alleles.

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MME JULIE FLAMENT

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Publications scientifiques (2) — classées par pathologie

Sjögren1

Transversal1

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