Linkage disequilibrium mapping places the gene causing familial Mediterranean fever close to D16S246

This report presents refined genetic mapping data for the gene causing familial Mediterranean fever (FMF), a recessively inherited disorder of inflammation. We sampled 65 Jewish, Armenian, and Arab families and typed them for eight markers from chromosome 16p. Using a new algorithm that permits mult...

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Veröffentlicht in:American journal of human genetics 1996-03, Vol.58 (3), p.523-534
Hauptverfasser: LEVY, E. N, YANG SHEN, GUMUCIO, D, PRAS, M, SHOHAT, M, ROTTER, J. I, FISCHEL-GHODSIAN, N, RICHARDS, R. I, KASTNER, D. L, KUPELIAN, A, KRUGLYAK, L, AKSENTIJEVICH, I, PRAS, E, BALOW, J. E, LINZER, B, XIAOGUANG CHEN, SHELTON, D. A
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Zusammenfassung:This report presents refined genetic mapping data for the gene causing familial Mediterranean fever (FMF), a recessively inherited disorder of inflammation. We sampled 65 Jewish, Armenian, and Arab families and typed them for eight markers from chromosome 16p. Using a new algorithm that permits multipoint calculations for a dense map of markers in consanguineous families, we obtained a maximal LOD score of 49.2 at a location 1.6 cM centromeric to D16S246. A specific haplotype at D16S283-D16S94-D16S246 was found in 76% of Moroccan and 32% of non-Moroccan Jewish carrier chromosomes, but this haplotype was not overrepresented in Armenian or Arab FMF carriers. Moreover, the 2.5-kb allele at D16S246 was significantly associated with FMF in Moroccan and non-Moroccan Jews but not in Armenians or Arabs. Since the Moroccan Jewish community represents a relatively recently established and genetically isolated founder population, we analyzed the Moroccan linkage-disequilibrium data by using Luria-Delbrück formulas and simulations based on a Poisson branching process. These methods place the FMF susceptibility gene within 0.305 cM of D16S246 (2-LOD-unit range 0.02-0.64 cM).
ISSN:0002-9297
1537-6605