MEFV mutations in systemic onset juvenile idiopathic arthritis

doi:10.1093/rheumatology/ken409

Rheumatology Advance Access published online on November 4, 2008
Rheumatology, doi:10.1093/rheumatology/ken409

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MEFV mutations in systemic onset juvenile idiopathic arthritis

N. A. Ayaz¹, S. Özen¹, Y. Bilginer¹, M. Ergüven², E. Ta $s$ k $i$ ran³, E. Y $i$ lmaz³, N. Be $s$ ba $s$ ¹, R. Topalo $g$ lu¹ and A. Bakkalo $g$ lu¹

¹Pediatric Nephrology and Rheumatology Unit, Hacettepe University Faculty of Medicine, Ankara, ²Pediatrics Department, Goztepe Education and Research Hospital, $I$ stanbul, and ³Medical Biology Unit, Hacettepe University Faculty of Medicine, Ankara, Turkey.

Correspondence to: S. Özen, Pediatric Nephrology and Rheumatology Unit, Hacettepe University Faculty of Medicine, 06100, Sihhiye, Ankara, Turkey. E-mail: sezaozen{at}hacettepe.edu.tr

Abstract

Objectives. Autoinflammatory diseases constitute a large spectrumof monogenic diseases like FMF or cryopyrin-associated periodicsyndromes (CAPS) and complex genetic trait diseases such assystemic onset juvenile idiopathic arthritis (SoJIA). An increasedrate of MEFV mutations has been shown among patients with PANand HSP, in populations where FMF is frequent. The aim of thestudy is to search for MEFV mutations in our patients with SoJIAand see whether these mutations had an effect on disease courseor complications.

Methods. Thirty-five children with the diagnosis of SoJIA werescreened for 12 MEFV mutations. The control data were obtainedfrom a previous study of our centre determining the carrierfrequency in Turkish population.

Results. Two patients were homozygous and three patients wereheterozygous for the M694V mutation. One patient was a compoundheterozygote for the M680I/V726A mutations. Heterozygous V726Amutation was found in one patient. The overall mutation frequencyof patients was 14.28%. This figure had been compared with thepreviously published rate of disease-causing mutations in thiscountry, which is 5%. Disease-causing mutations were found tobe significantly more frequent in the SoJIA patients than thepopulation (P < 0.01). Among these, M694V was the leadingmutation with a frequency of 10% in SoJIA. Six patients carryingMEFV mutations were among the most resistant cases requiringbiological therapy.

Conclusion. SoJIA patients had a significantly higher frequencyof MEFV mutations but clinical studies with large number ofpatients are needed to confirm the association of MEFV mutationswith SoJIA and its course.

KEY WORDS: Familial Mediterranean fever, Systemic onset juvenile idiopathic arthritis, Mediteranean fever, Mutation

Submitted 22 May 2008; Accepted 19 September 2008

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