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Diagnostic and Therapeutic Insights From a Cohort of Chronic Recurrent Multifocal Osteomyelitis (Crmo) Patients Publisher



Ka Ashari Kosar ASNA ; Ms Mousavi Mahdieh SADAT ; F Tahghighi FATEMEH ; R Assari RAHELEH ; Sr Raeeskarami Seyed REZA ; V Ziaee VAHID
Authors

Source: BMC Rheumatology Published:2025


Abstract

Background: Chronic recurrent multifocal osteomyelitis (CRMO) is a sporadic form of autoinflammatory bone disorders (ABDs) presenting with sterile chronic and/or recurrent and multiple sites of bone involvement. We aimed to describe our 10-year cohort of CRMO patients and analyze the characteristics and treatment approaches. Methods: We retrospectively analyzed the data on patients with bone diseases at Children’s Medical Center, Tehran University of Medical Sciences, Iran in the previous 10 years. The criteria for inclusion of patients as CNO/CRMO were mono-, oligo- or multifocal inflammatory bone lesions (osteomyelitis, osteitis, osteosclerosis) by imaging techniques; duration of complaints for > 6 weeks; and onset before 18 years of age. Results: Thirty-nine patients were enrolled. Diagnosis of five patients were found compatible with monogenic ABDs. There were four sites of bone involvement per patient. The most common sites were vertebrae, pelvis, and tibia. Eight patients (23%) had dermatologic manifestations, including three psoriasis cases and one palmar pustulosis. All patients received NSAIDs, and 85% received it as first-line. Treatment was escalated to methotrexate or prednisolone when response was suboptimal. Out of 17 patients primarily treated only with NSAIDs, 47% remitted. In general, 84% of our patients are in remission: 36% without medication and 48% with medication. Conclusion: Our CRMO patients showed an acceptable remission response to the current treatment regimen. Results of bone scintigraphy in suspected CRMO patients should be interpreted cautiously as an adjunct to clinical investigations. Special attention should be paid to extraosseous manifestations in suspected CRMO patients to avoid overlooking monogenic ABDs. Clinical trial number: Not applicable. © 2025 Elsevier B.V., All rights reserved.