AI Article Synopsis

  • The study investigates the use of disease-modifying drugs (DMDs) as a treatment for idiopathic sclerosing orbital inflammatory syndrome (ISOIS), a rare and challenging condition.
  • Conducted at a university hospital, it involved five biopsy-confirmed patients, whose disease activity was monitored using systematic criteria and treated with a combination of anti-TNF alpha agents, azathioprine, and low-dose corticosteroids.
  • Results showed that all patients experienced a decrease in disease activity over an average follow-up of nearly 33 months, suggesting that biologic DMDs could effectively manage ISOIS and potentially alter its progression.

Article Abstract

Purpose: Idiopathic sclerosing orbital inflammatory syndrome (ISOIS) is a rare, progressive and hard to control disease. There is a deep gap of evidence regarding application of disease-modifying drugs (DMD) regimen as a potentially effective treatment for orbital inflammatory diseases. We aimed to report the results of using DMDs and discuss the concept of applying this modality of treatment in patients with ISOIS.

Methods: This was a prospective interventional case series conducted in a tertiary university-based hospital. Biopsy proven patients with active ISOIS were included. Systematic criteria were developed to define and measure disease activity and monitor response to treatment. A DMD regimen including an anti-tumor necrosis factor alpha (anti-TNF alpha) agent plus azathioprine and low-dose corticosteroids were used. Comprehensive ophthalmic, orbital and systemic assessments were performed during each visit.

Results: Five eligible patients with primary ISOIS were included. Mean age was 34.20 (SD = 13.33, range 19-53) years. Three had unilateral and two had bilateral involvement. Four had diffuse orbital involvement pattern and progressive worsening of visual functions, reduced extraocular motility and proptosis. In one patient the disease was localized to extraocular muscle and lacrimal gland. Disease activity was decreased and stabilized after DMDs regimen in all patients. Mean follow up was 32.80 (SD = 30.80, range: 12-86) months.

Conclusion: Biologic DMD (b-DMD) including anti-TNF alpha, corticosteroid and azathioprine were effective in decreasing disease activity and could change course of the disease. This study supports the concept of using b-DMD regimen in treatment of ISOIS.

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Source
http://dx.doi.org/10.1080/01676830.2021.1929338DOI Listing

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