TY - JOUR
T1 - Clinical and imaging outcomes of different phenotypes of axial spondyloarthritis
T2 - 5-year analysis of the DESIR cohort
AU - Sepriano, Alexandre
AU - Ramiro, Sofia
AU - van der Heijde, Désirée
AU - Moltó, Anna
AU - Gaujoux-Viala, Cécile
AU - Dougados, Maxime
AU - Landewé, Robert
N1 - Funding Information:
The DESIR study is under the umbrella of the French Society of Rheumatology, which financially supports the cohort. The DESIR cohort is run with the support of unrestricted grants from (in order of decreasing support) Pfizer France, Biogen, AbbVie, UCB, Lilly, Galapagos, Novartis, MSD, Fresenius and Celltrion HealthCare.
Funding Information:
The DESIR cohort is conducted with Assistance Publique-Hopitaux de Paris (AP-HP, Paris France) as the sponsor and under the umbrella of the French Society of Rheumatology. The DESIR cohort is run with the support of unrestricted grants from (in order of decreasing support) Pfizer France, Biogen, AbbVie, UCB, Lilly, Galapagos, Novartis, MSD, Fresenius and Celltrion HealthCare. We thank the Clinical Research Unit Paris Centre (AP-HP, Paris France), and the Institut national de la sante et de la recherche medicale (Inserm). We also thank the investigators: Pr Maxime Dougados, Pr André Kahan, Dr Julien Wipff and Dr Anna Moltó (Paris-Cochin), Pr Olivier Meyer, Pr Philippe Dieudé (Paris-Bichat), Pr Pierre Bourgeois, Pr Laure Gossec (Paris-La Pitie-Salpétriere), Pr Francis Berenbaum (Paris-Saint-Antoine), Pr Pascal Claudepierre (Creteil), Pr Maxime Breban, Pr Maria-Antonietta D'Agostino, Pr Félicie Costantino (Boulogne-Billancourt), Pr Michel De Bandt, Dr Bernadette Saint-Marcoux (Aulnay-sous-Bois), Pr Philippe Goupille (Tours), Pr Jean-Françis Maillefert (Dijon), Pr Xavier Puechal, Dr Emmanuelle Dernis (Le Mans), Pr Daniel Wendling, Pr Clément Prati (Besançon), Pr Bernard Combe, Pr Cédric Lukas (Montpellier), Pr Liana Euller-Ziegler, Pr Véronique Breuil (Nice), Pr Pascal Richette (Paris Lariboisière), Pr Pierre Lafforgue, Pr Thao Pham (Marseille), Pr Patrice Fardellone, Dr Patrick Boumier, Dr Pauline Lasselin (Amiens), Pr Jean-Michel Ristori, Pr Martin Soubrier, Pr Anne Tournadre (Clermont-Ferrand), Dr Nadia Mehsen (Bordeaux), Pr Damien Loeuille (Nancy), Pr Rene-Marc Flipo (Lille), Pr Alain Saraux (Brest), Pr Corinne Miceli, Dr Stephan Pavy (Le Kremlin-Bicêtre), Pr Alain Cantagrel, Pr Adeline Ruyssen-Witrand (Toulouse), Pr Olivier Vittecoq, Pr Thierry Lequerre (Rouen).
Publisher Copyright:
© 2024 Elsevier Inc.
PY - 2024/6
Y1 - 2024/6
N2 - Objectives: To compare the long-term outcomes of three phenotypes of axial SpA (axSpA). Methods: Patients with a clinical diagnosis of axSpA from the DESIR cohort were grouped into three phenotypes at baseline: ‘Pure axSpA’ (‘Axial’), ‘axSpA with peripheral signs’ (‘IBP+Peripheral’) and ‘axSpA at risk’ (‘At risk’) by latent class analysis. Clinical and imaging data were collected up to 5 years. Clinical outcomes, measured in each visit, included disability (BASFI) and quality of life (QoL; SF36). Imaging outcomes included inflammatory and structural lesions on MRI and radiographs of spine and SIJ. The association between phenotype membership at baseline and each outcome was tested in multivariable GEE models. Results: In total, 576 patients with axSpA were included. ‘At risk’ patients had worse disability and QoL than ‘Axial’ patients over time. For instance, ‘At risk’ patients had on average 0.4 more points in BASFI over time than ‘Axial’ patients [β (95 % CI): 0.4 (0.2; 0.7)]. This difference was mostly noted in female patients who were HLA-B27 positive. In addition, the difference between the ‘At risk’ and ‘Axial’ phenotypes was higher in patients receiving bDMARDs than in those not (β=0.6 vs 0.5), since BASFI improved more in ‘Axial’ (∆BASFI: -1.3) than in ‘At risk’ (∆BASFI: -0.9) treated patients. There were no differences in disability and QoL between ‘Axial’ and ‘IBP+Peripheral’ patients. Imaging outcomes were worse in the ‘Axial’ phenotype than in the others over time. Conclusion: Patients with ‘axSpA at risk’ show worse self-reported outcomes over time and are less likely to benefit from anti-inflammatory treatment than those with a classical axSpA phenotype.
AB - Objectives: To compare the long-term outcomes of three phenotypes of axial SpA (axSpA). Methods: Patients with a clinical diagnosis of axSpA from the DESIR cohort were grouped into three phenotypes at baseline: ‘Pure axSpA’ (‘Axial’), ‘axSpA with peripheral signs’ (‘IBP+Peripheral’) and ‘axSpA at risk’ (‘At risk’) by latent class analysis. Clinical and imaging data were collected up to 5 years. Clinical outcomes, measured in each visit, included disability (BASFI) and quality of life (QoL; SF36). Imaging outcomes included inflammatory and structural lesions on MRI and radiographs of spine and SIJ. The association between phenotype membership at baseline and each outcome was tested in multivariable GEE models. Results: In total, 576 patients with axSpA were included. ‘At risk’ patients had worse disability and QoL than ‘Axial’ patients over time. For instance, ‘At risk’ patients had on average 0.4 more points in BASFI over time than ‘Axial’ patients [β (95 % CI): 0.4 (0.2; 0.7)]. This difference was mostly noted in female patients who were HLA-B27 positive. In addition, the difference between the ‘At risk’ and ‘Axial’ phenotypes was higher in patients receiving bDMARDs than in those not (β=0.6 vs 0.5), since BASFI improved more in ‘Axial’ (∆BASFI: -1.3) than in ‘At risk’ (∆BASFI: -0.9) treated patients. There were no differences in disability and QoL between ‘Axial’ and ‘IBP+Peripheral’ patients. Imaging outcomes were worse in the ‘Axial’ phenotype than in the others over time. Conclusion: Patients with ‘axSpA at risk’ show worse self-reported outcomes over time and are less likely to benefit from anti-inflammatory treatment than those with a classical axSpA phenotype.
KW - Axial spondyloarthritis
KW - Phenotypes
KW - Prognosis
UR - http://www.scopus.com/inward/record.url?scp=85187540122&partnerID=8YFLogxK
U2 - 10.1016/j.semarthrit.2024.152424
DO - 10.1016/j.semarthrit.2024.152424
M3 - Article
C2 - 38479110
AN - SCOPUS:85187540122
SN - 0049-0172
VL - 66
JO - Seminars in Arthritis and Rheumatism
JF - Seminars in Arthritis and Rheumatism
M1 - 152424
ER -