Non-founder mutations in the MEFV gene establish this gene as the cause of familial Mediterranean fever (FMF)

Bernot, Alain; Silva, Corinne Da; Petit, Jean-Louis; Cruaud, Corinne; Caloustian, Christophe; Castet, Valérie; Ahmed-Arab, Mehdi; Dross, Christiane; Dupont, Madeleine; Cattan, D; Smaoui, Nizar; Dodé, Catherine; Pécheux, Christophe; Nédelec, Brigitte; Medaxian, Jean; Rozenbaum, M; Rosner, I; Delpech, Marc; Grateau, Gilles; Demaille, Jacques; Weissenbach, Jean; Touitou, Isabelle

doi:10.1093/hmg/7.8.1317

Cited by 227 publications

(171 citation statements)

References 23 publications

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“…11 Patient samples were then tested for the 12 most common mutations within the Armenian population. The FMF StripAssay, 12,13 which is based on the reversehybridization principle, was used to identify the following 12 MEFV mutations: E148Q, P369S, F479L, M680I (G/C), M680I (G/A), I692del, M694V, M694I, K695R, V726A, A744S and R761H. A total of 63 samples, 20 homozygous or compound heterozygous, 23 heterozygous and 20 asymptomatic wild-type controls, were selected and their MEFV gene was completely sequenced independently in the United States using dideoxy termination methodology on an ABI 3100 capillary electrophoresis instrument (Appliedbiosystems Inc., Carlsbad, CA, USA).…”

Section: Methodsmentioning

confidence: 99%

Genotype–phenotype studies in a large cohort of Armenian patients with familial Mediterranean fever suggest clinical disease with heterozygous MEFV mutations

et al. 2010

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Familial Mediterranean fever (FMF) is an autoinflammatory disorder generally caused by recessively inherited mutations in the MEFV gene. FMF is quite prevalent in Armenian population in which majority of patients have two mutated alleles, yet in 18% of symptomatic patients just one mutation has been detected. To explain this finding, we analyzed the symptoms and genotypes of 1299 patients, including 236 affected heterozygous patients with definite diagnosis of FMF. We selected a subset of 63 heterozygous, homozygous and asymptomatic normal individuals and completely sequenced their MEFV genes (exons) to discover any other mutations potentially missed by currently used screening method. Besides four synonymous polymorphisms in exon two and five, we found a T267I mutation in one heterozygous patient with a severe case of FMF who should have been designated as compound heterozygous, yet the other genotypes were all accurate. We used binomial probability distribution of symptoms in homozygous FMF patients to estimate the likelihood of their occurrences in heterozygous patients and demonstrated the assemblage of patients into groups with similar clinical criteria using statistical clustering. We found extremely high probabilities for the presence of FMF symptoms in heterozygous individuals and determined that symptoms were equally likely to occur in both analyzed genotypes. Therefore, our study supports the rising evidence that a single MEFV mutation could be associated with mild FMF symptoms. However, heterozygous patients presenting with severe phenotype should be further analyzed for less common second MEFV mutation using gene sequencing.

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Section: Methodsmentioning

confidence: 99%

Genotype–phenotype studies in a large cohort of Armenian patients with familial Mediterranean fever suggest clinical disease with heterozygous MEFV mutations

et al. 2010

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“…For example, we were able to phase two genes that contained more than two nonsynonymous, heterozygous alleles known to be associated with recessive diseases (Supplementary Table 21). Variants in MEFV 18 and ADAMTS13 (ref. 19), which are predicted to cause familial Mediterranean fever and Upshaw-Shalman syndrome under the autosomal recessive inheritance pattern, respectively, were found in cis configuration, with the partner haplotype left intact.…”

Section: Letter Researchmentioning

confidence: 99%

De novo assembly and phasing of a Korean human genome

Seo

Rhie

Kim

et al. 2016

Nature

305

301

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Although massively parallel sequencing approaches have been widely used to study genomic variation, simple alignment of short reads to a reference genome cannot be used to investigate the full range of structural variation and phased diploid architecture, which are important for precision medicine. By contrast, the single-molecule real-time (SMRT) sequencing platform produces long reads that can resolve repetitive structures effectively. We integrated this technology with several other sequencing approaches to construct a high-quality

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“…Subsequently, the p.E148Q sequence alteration was identified on exon 2 (19). These were found to be the most common mutations among the populations of the countries where FMF is prevalent.…”

Section: Distribution Of Mefv Mutations In Fmf Patients Around the Worldmentioning

confidence: 99%

Familial Mediterranean Fever in the World

Ben-Chétrit¹,

Touitou²

2009

Arthritis & Rheumatism

350

262

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Non-founder mutations in the MEFV gene establish this gene as the cause of familial Mediterranean fever (FMF)

Cited by 227 publications

References 23 publications

Genotype–phenotype studies in a large cohort of Armenian patients with familial Mediterranean fever suggest clinical disease with heterozygous MEFV mutations

Genotype–phenotype studies in a large cohort of Armenian patients with familial Mediterranean fever suggest clinical disease with heterozygous MEFV mutations

De novo assembly and phasing of a Korean human genome

Familial Mediterranean Fever in the World

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