par Ciregia, Federica;Baiwir, Dominique;Cobraiville, Gaël;Dewael, Thibaut;Mazzucchelli, Gabriel;Badot, Valérie 
;Di Romana, Silvana ;Sidiras, Paschalis ;Sokolova, T.;Durez, Patrick ;Malaise, Michel;De Seny, Dominique
Référence Journal of translational medicine, 18, 1, 8
Publication Publié, 2020-01
;Di Romana, Silvana ;Sidiras, Paschalis ;Sokolova, T.;Durez, Patrick ;Malaise, Michel;De Seny, DominiqueRéférence Journal of translational medicine, 18, 1, 8
Publication Publié, 2020-01
Article révisé par les pairs
| Résumé : | Background: Serum protein glycosylation is an area of investigation in inflammatory arthritic disorders such as rheumatoid arthritis (RA). Indeed, some studies highlighted abnormalities of protein glycosylation in RA. Considering the numerous types of enzymes, monosaccharides and glycosidic linkages, glycosylation is one of the most complex post translational modifications. By this work, we started with a preliminary screening of glycoproteins in serum from RA patients and controls. Methods: In order to isolate glycoproteins from serum, lectin wheat germ agglutinin was used and quantitative differences between patients and controls were investigated by LC-MS/MS. Consequently, we focused our attention on two glycoproteins found in this explorative phase: corticosteroid-binding globulin (CBG) and lipopolysaccharide-binding protein (LBP). The subsequent validation with immunoassays was widened to a larger number of early RA (ERA) patients (n = 90) and well-matched healthy controls (n = 90). Results: We observed a significant reduction of CBG and LBP glycosylation in ERA patients compared with healthy controls. Further, after 12 months of treatment, glycosylated CBG and LBP levels increased both to values comparable to those of controls. In addition, these changes were correlated with clinical parameters. Conclusions: This study enables to observe that glycosylation changes of CBG and LBP are related to RA disease activity and its response to treatment. |
