Bernot A, da Silva C, Petit J L, Cruaud C, Caloustian C, Castet V, Ahmed-Arab M, Dross C, Dupont M, Cattan D, Smaoui N, Dodé C, Pêcheux C, Nédelec B, Medaxian J, Rozenbaum M, Rosner I, Delpech M, Grateau G, Demaille J, Weissenbach J, Touitou I
Généthon, CNRS-URA1922, 91000 Evry, France.
Hum Mol Genet. 1998 Aug;7(8):1317-25. doi: 10.1093/hmg/7.8.1317.
Familial Mediterranean fever (FMF) is an autosomal recessive disorder characterized by recurring attacks of fever and serositis. It affects primarily North African Jews, Armenians, Turks and Arabs, in which a founder effect has been demonstrated. The marenostrin-pyrin-encoding gene has been proposed as a candidate gene for the disease ( MEFV ), on the basis of the identification of putative mutations clustered in exon 10 (M680V, M694I, M694V and V726A), each segregating with one ancestral haplotype. In a search for additional MEFV mutations in 120 apparently non-founder FMF chromosomes, we observed eight novel mutations in exon 2 (E148Q, E167D and T267I), exon 5 (F479L) and exon 10 (I692del K695R, A744S and R761H). Except for E148Q and K695R, all mutations were found in a single chromosome. Mutation E148Q was found in all ethnic groups studied and in association with a novel ancestral haplotype in non-Ashkenazi Jews (S2). Altogether, these new findings definitively establish the marenostrin/pyrin-encoding gene as the MEFV locus.
家族性地中海热(FMF)是一种常染色体隐性疾病,其特征为发热和浆膜炎反复发作。它主要影响北非犹太人、亚美尼亚人、土耳其人和阿拉伯人,在这些人群中已证实存在奠基者效应。基于在外显子10中聚集的假定突变(M680V、M694I、M694V和V726A)的鉴定,每个突变都与一种祖先单倍型分离,编码marenostrin-吡喃的基因已被提议作为该疾病的候选基因(MEFV)。在对120条明显非奠基者的FMF染色体进行的额外MEFV突变搜索中,我们在外显子2(E148Q、E167D和T267I)、外显子5(F479L)和外显子10(I692del K695R、A744S和R761H)中观察到8个新突变。除E148Q和K695R外,所有突变均在一条染色体上发现。突变E148Q在所有研究的种族群体中均有发现,并且与非阿什肯纳兹犹太人中的一种新的祖先单倍型(S2)相关。总之,这些新发现明确地将编码marenostrin/吡喃的基因确定为MEFV基因座。
