A decision tree for genetic diagnosis of hereditary periodic fever in unselected patients

Background: The diagnostic value of molecular analysis of the familial Mediterranean fever (FMF) gene (Mediterranean fever (MEFV)) has been well established only in patients selected on the basis of ethnic background or clinical criteria. Genetic diagnosis for other hereditary periodic fever syndrom...

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Bibliographic Details
Published in:Annals of the rheumatic diseases 2006-11, Vol.65 (11), p.1427-1432
Main Authors: Federici, L, Rittore-Domingo, C, Koné-Paut, I, Jorgensen, C, Rodière, M, Le Quellec, A, Touitou, I
Format: Article
Language:English
Subjects:
Abdomen
Adolescent
Adult
Biological and medical sciences
CAPS
Child
Child, Preschool
cryopyrin-associated periodic syndrome
Cytokines
Cytoskeletal Proteins - genetics
Decision Trees
Diagnosis, Differential
Disease
Diseases of the osteoarticular system
DNA Mutational Analysis - methods
Extended Report
familial cold urticaria
familial Mediterranean fever
Familial Mediterranean Fever - diagnosis
Familial Mediterranean Fever - ethnology
Familial Mediterranean Fever - genetics
FCU
Female
Fever
FMF
Gangrene
Genes
Genotype
HIDS
Humans
hyperimmunoglobulinaemia D syndrome
Laboratories
Male
Medical sciences
Mediterranean fever
MEFV
Middle Aged
Mutation
Patients
PCR
polymerase chain reaction
Pyrin
Retrospective Studies
Sensitivity and Specificity
TRAPS
Tumor necrosis factor-TNF
tumour necrosis factor receptor-associated periodic syndrome
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Description
Summary:Background: The diagnostic value of molecular analysis of the familial Mediterranean fever (FMF) gene (Mediterranean fever (MEFV)) has been well established only in patients selected on the basis of ethnic background or clinical criteria. Genetic diagnosis for other hereditary periodic fever syndromes has been poorly evaluated. Objective: To determine the diagnostic contribution of genetic tests for hereditary periodic syndromes in a large, unselected series of patients. Methods: A retrospective study was conducted on 1941 patients referred to us for FMF genetic tests between 1997 and 2005. MEFV genotypes were compared with clinical data to appraise criteria for FMF diagnosis. Genetic tests for tumour necrosis factor receptor-associated periodic syndrome (TRAPS), hyperimmunoglobulinaemia D syndrome (HIDS) and cryopyrin-associated periodic syndromes (CAPS) were also reviewed. Results: 71% of the 1574 patients with enough data had a clinical diagnosis of FMF according to the widely used Israeli criteria. Two MEFV mutations were found in only 409 patients of this subgroup (sensitivity = 37%) and in 15 (3.3%) of the patients with an improbable clinical diagnosis of FMF (specificity = 97%). Molecular diagnosis for alternate hereditary periodic syndromes was carried out in 456 of the patients having a non-conclusive FMF genetic test. A positive diagnosis was obtained in 31 of these patients (TRAPS (n = 19), HIDS (n = 4) and CAPS (n = 8)). Conclusions: First-line MEFV mutation screening in patients with clinically typical FMF may be appropriate only in particular areas. To optimise genetic diagnosis, we propose a decision tree, which, with the advice of an expert practitioner, could help redirect test indications towards non-FMF hereditary periodic syndromes.
ISSN:0003-4967
1468-2060
DOI:10.1136/ard.2006.054304