LAUSR

Objectives To explore and compare the prevalences of a wide range of comorbidities in axial spondyloarthritis (axSpA) versus the general population, and in non-radiographic versus radiographic axSpA (nr-axSpA/r-axSpA). Method Well-characterized axSpA patients (n = 246) from the SPARTAKUS cohort (55% men; mean age/disease duration 52/26 years; nr-axSpA/r-axSpA = 82/164) were included, and matched to comparators from the general population (five/patient) randomly drawn from the Swedish Population Register. Fifty-nine comorbidities were determined from ICD-10 diagnosis registrations in primary/specialized care, with data retrieved for the 10 year period preceding SPARTAKUS inclusion (for patients/their respective comparators). Differences in comorbidity prevalences were analyzed using logistic regression and controlled for multiple comparisons. Results Most investigated comorbidities were numerically overrepresented in axSpA versus comparators with significantly higher prevalences of known extra-musculoskeletal manifestations [anterior uveitis (28% vs 1%), IBD (10%/1%), psoriasis (10%/3%)], and ischaemic heart disease (7%/3%), along with less explored conditions such as fibromyalgia/chronic pain (12%/3%) and nephrolithiasis (8%/3%). Patients displayed significantly higher proportions of well-known side-effects of non-steroidal anti-inflammatory drugs (NSAIDs) [gastritis (21%/10%), hypertension (31%/19%)] and glucocorticoids [cataract (11%/7%), glaucoma (7%/3%), osteoporosis/vertebral compression (4%/1%)]. No significant between-group difference (patients/comparators) was observed for Charlson Comorbidity Index (assessing short-term mortality risk) when excluding rheumatic disease. Moreover, no significant difference in comorbidity was found between nr-axSpA and r-axSpA. Conclusion axSpA is linked to several comorbidities, whereas no difference was observed between nr-axSpA and r-axSpA. Potential causes of enhanced comorbidity include long-standing inflammation and therapy side-effects (including from NSAIDs/glucocorticoids), both to be considered when aiming to optimize axSpA treatment.