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American Journal of Human Genetics logoLink to American Journal of Human Genetics
. 1998 Oct;63(4):1095–1101. doi: 10.1086/302062

A gene for Meckel syndrome maps to chromosome 11q13.

J Roume 1, E Genin 1, V Cormier-Daire 1, H W Ma 1, B Mehaye 1, T Attie 1, F Razavi-Encha 1, C Fallet-Bianco 1, A Buenerd 1, F Clerget-Darpoux 1, A Munnich 1, M Le Merrer 1
PMCID: PMC1377494  PMID: 9758620

Abstract

Meckel syndrome (MKS) is a rare autosomal recessive lethal condition of unknown origin, characterized by (i) an occipital meningo-encephalocele with (ii) enlarged kidneys, with multicystic dysplasia and fibrotic changes in the portal area of the liver and with ductal proliferation, and (iii) postaxial polydactyly. A gene responsible for MKS in Finland has been mapped to chromosome 17q21-q24. Studying a subset of Middle Eastern and northern African MKS families, we have recently excluded the chromosome 17 region and have suggested a genetic heterogeneity. In the present study, we report on the mapping of a second MKS locus (MKS2) to chromosome 11q13, by homozygosity mapping in seven families that do not show linkage to chromosome 17q21-q24 (maximum LOD score 4.41 at recombination fraction .01). Most interestingly, the affected fetuses of southern Tunisian ancestry shared a particular haplotype at loci D11S911 and D11S906, suggesting that a founder effect is involved. Our observation gives support to the clinical and genetic heterogeneity of MKS.


Articles from American Journal of Human Genetics are provided here courtesy of American Society of Human Genetics

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