German Center for Pediatric and adolescent Rheumatology, Hospital Garmisch-Partenkirchen, Garmisch-Partenkirchen, Germany
Elisabeth Weissbarth-Riedel
Department of Pediatrics, University Medical Center Hamburg-Eppendorf, Hamburg, Germany
Christoph Rietschel
Kinder- und Jugendrheumatologie, Clementine Children`s Hospital—Dr Christ`sche Foundation, Frankfurt am Main, Germany
Rainer Berendes
Pediatric Rheumatology, Children`s Hospital St. Marien, Landshut, Germany
Prasad Oommen
Department of Pediatric Oncology, Hematology and Clinical Immunology, Division of Pediatric Rheumatology, Heinrich-Heine-Universitat Dusseldorf, Dusseldorf, Germany
Claas Hinze
Pediatric Rheumatology and Immunology, University Medicine, Albert-Schweitzer-Campus 1, Munster, Germany
Inès Elhani
Department of General Pediatrics, Hospital Centre Versailles, Le Chesnay, France
Stefan Backes
Pediatric Rheumatology and Immunology, University Medicine, Albert-Schweitzer-Campus 1, Munster, Germany
Sabrina Fühner
Pediatric Rheumatology and Immunology, University Medicine, Albert-Schweitzer-Campus 1, Munster, Germany
Arnd Giese
Department of Internal Medicine I, Marienhospital Herne Medical Center of Ruhr University Bochum, Herne, Germany
Anna Lisa Hitzegrad
Charité University Medicine Berlin, Social Pediatric Center, Berlin, Germany
Annette Jansson
Division of Pediatric Rheumatology and Immunology, Department of Pediatrics, University Hospital of Munich, Munchen, Germany
Katerina Theodoropoulo
Département Femme-Mère-Enfant (DFME), Unité Romande d`Immuno-rhumatologie Pédiatrique (URIRP), CHUV, University of Lausanne, Lausanne, Switzerland
Introduction Familial Mediterranean fever (FMF) is a genetic disease leading to recurrent episodes of inflammation. Two pathogenic variants are required for classical disease, but the disease can occur in heterozygous patients. Patients are treated continuously with colchicine to prevent amyloid A (AA) amyloidosis, including heterozygous patients who display a moderate form of FMF and rarely develop AA amyloidosis. The need for lifelong colchicine treatment in heterozygous FMF is therefore controversial. We aimed to characterise genotype-specific levels of inflammatory biomarkers, and to focus on heterozygous patients who discontinued colchicine.Methods All patients with FMF from the European databases AIDnet and JIRcohort who received colchicine during follow-up were included. Demographics, C reactive protein (CRP), serum amyloid A (SAA), S100A8/A9 and S100A12 levels, leucocyte and neutrophil counts were extracted. Visits were classified as active, subclinical or inactive according to symptoms, CRP and SAA levels.Results Data from 747 patients were extracted (233 homozygous, 201 compound heterozygous, 224 heterozygous patients, 49 heterozygous with one class III variant and 40 compound heterozygous with two class III variants). During active visits, all biomarker levels were higher compared with inactive visits (p<0.001). Heterozygous patients showed lower levels of CRP, SAA, S100A8/A9 and S100A12 during inactive and subclinical visits than patients with two class IV-V variants. Colchicine was discontinued in 52 heterozygous patients and reintroduced in 23 of them (44%).Conclusion S100A8/A9 and S100A12 proteins are biomarkers that can be used to assess disease activity. Heterozygous patients have lower levels of inflammatory biomarkers and some of them can sustainably discontinue colchicine treatment.
