AI Article Synopsis

  • - The study followed 175 patients with idiopathic inflammatory myositis (IIM) for an average of about 65 months, documenting their treatment responses, functional outcomes, and overall health at the end of follow-up.
  • - Results showed that 74.1% of patients experienced a complete clinical response, while 40.2% were able to stop steroid treatment and 13.8% achieved clinical remission, with better outcomes linked to full responses.
  • - The study concluded that most myositis subsets had favorable long-term outcomes, but partial responses led to poorer functional results and increased damage, with a notable early mortality rate primarily tied to active disease.

Article Abstract

Background: We report a longitudinal observational cohort of idiopathic inflammatory myositis (IIM) focusing on the long-term clinical outcome and associated parameters.

Methods: IIM patients were classified as per Bohan and Peter criteria. In those with ≥ 24 months of follow-up; the treatment response, functional outcomes, and damage at last follow-up were recorded. Complete clinical response and clinical remission as defined by Oddis et al., was used to define outcomes at last follow-up.

Results: The cohort consists of 175 patients, mean age 40.9 (+12.6) years, M:F 1:3.3; and the major subsets were dermatomyositis (44.6%), overlap myositis (25.7%), antisynthetase syndrome (6.3%), polymyositis (14.3%), and juvenile DM/OM (8.6%). Ninety-four patients have followed up for 24 months or more, with the median (IQR) of 65(35,100.7) months. Of them, 74.1% and 11.8% had complete and partial clinical responses respectively at the last follow-up. In our cohort 40.2% were off-steroids and 13.8% were in clinical remission at the last follow-up. Complete clinical response was associated with better functional outcomes and lesser damage as determined by HAQ-DI of 0[OR10.9; 95%CI (3.3,160)], MRS [OR 3.2; 95%CI (1.4,7.3)] and lesser MDI [OR 1.7; 95% CI (1.1,2.7)] respectively as compared to partial response (unadjusted analysis). Baseline parameters and IIM subsets did not significantly influence the functional outcome and damage. The mortality rate in our cohort is 24/175 (13.7%), the disease-specific mortality rate being 9.1%. Large majority of deaths were early, associated with active disease.

Conclusion: We report good long-term outcomes in all major myositis subsets. Partial clinical response to treatment is associated with worse functional outcomes and damage accrual. Death occurs early in association with active disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10815524PMC
http://dx.doi.org/10.31138/mjr.280823.ltoDOI Listing

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