Genetic and mutational analyses of a large multiethnic Bardet-Biedl cohort reveal a minor involvement of BBS6 and delineate the critical intervals of other loci.

Bardet-Biedl syndrome (BBS) is a rare autosomal recessive disorder characterized primarily by obesity, polydactyly, retinal dystrophy, and renal disease. The significant genetic and clinical heterogeneity of this condition have substantially hindered efforts to positionally clone the numerous BBS genes, because the majority of available pedigrees are small and the disorder cannot be assigned to any of the six known BBS loci. Consequently, the delineation of critical BBS intervals, which would accelerate the discovery of the underlying genetic defect(s), becomes difficult, especially for loci with minor contributions to the syndrome. We have collected a cohort of 163 pedigrees from diverse ethnic backgrounds and have evaluated them for mutations in the recently discovered BBS6 gene (MKKS) on chromosome 20 and for potential assignment of the disorder to any of the other known BBS loci in the human genome. Using a combination of mutational and haplotype analysis, we describe the spectrum of BBS6 alterations that are likely to be pathogenic; propose substantially reduced critical intervals for BBS2, BBS3, and BBS5; and present evidence for the existence of at least one more BBS locus. Our data also suggest that BBS6 is a minor contributor to the syndrome and that some BBS6 alleles may act in conjunction with mutations at other BBS loci to cause or modify the BBS phenotype.

[1]  V. Sheffield,et al.  Mutations in MKKS cause Bardet-Biedl syndrome , 2001, Nature Genetics.

[2]  Richard A. Lewis,et al.  Mutations in MKKS cause obesity, retinal dystrophy and renal malformations associated with Bardet-Biedl syndrome , 2000, Nature Genetics.

[3]  G. Bouffard,et al.  Mutation of a gene encoding a putative chaperonin causes McKusick-Kaufman syndrome , 2000, Nature Genetics.

[4]  J. Lupski,et al.  Delineation of the critical interval of Bardet-Biedl syndrome 1 (BBS1) to a small region of 11q13, through linkage and haplotype analysis of 91 pedigrees. , 1999, American journal of human genetics.

[5]  M. Woods,et al.  A founder effect in the newfoundland population reduces the Bardet-Biedl syndrome I (BBS1) interval to 1 cM. , 1999, American journal of human genetics.

[6]  P. Beales,et al.  New criteria for improved diagnosis of Bardet-Biedl syndrome: results of a population survey , 1999, Journal of medical genetics.

[7]  M. Woods,et al.  A fifth locus for Bardet-Biedl syndrome maps to chromosome 2q31. , 1999, American journal of human genetics.

[8]  M. Woods,et al.  Genetic heterogeneity of Bardet-Biedl syndrome in a distinct Canadian population: evidence for a fifth locus. , 1999, Genomics.

[9]  M. Woods,et al.  Canadian Bardet-Biedl syndrome family reduces the critical region of BBS3 (3p) and presents with a variable phenotype. , 1998, American journal of medical genetics.

[10]  M Jay,et al.  Linkage mapping in 29 Bardet-Biedl syndrome families confirms loci in chromosomal regions 11q13, 15q22.3-q23, and 16q21. , 1997, Genomics.

[11]  G. Hitman,et al.  Bardet-Biedl syndrome: a molecular and phenotypic study of 18 families. , 1997, Journal of medical genetics.

[12]  V. Sheffield,et al.  Phenotypic differences among patients with Bardet-Biedl syndrome linked to three different chromosome loci. , 1995, American journal of medical genetics.

[13]  V. Sheffield,et al.  Use of a DNA pooling strategy to identify a human obesity syndrome locus on chromosome 15. , 1995, Human molecular genetics.

[14]  V. Sheffield,et al.  Identification of a Bardet-Biedl syndrome locus on chromosome 3 and evaluation of an efficient approach to homozygosity mapping. , 1994, Human molecular genetics.

[15]  J. Lupski,et al.  Bardet–Biedl syndrome is linked to DNA markers on chromosome 11 q and is genetically heterogeneous , 1994, Nature Genetics.

[16]  V. Sheffield,et al.  Linkage of Bardet–Biedl syndrome to chromosome 16q and evidence for non–allelic genetic heterogeneity , 1993, Nature Genetics.

[17]  A. Teebi,et al.  High incidence of Bardet Biedl syndrome among the Bedouin , 1989, Clinical genetics.

[18]  W. Pryse-Phillips,et al.  The cardinal manifestations of Bardet-Biedl syndrome, a form of Laurence-Moon-Biedl syndrome. , 1989, The New England journal of medicine.

[19]  D. Klein,et al.  The syndrome of Laurence-Moon-Bardet-Biedl and allied diseases in Switzerland. Clinical, genetic and epidemiological studies. , 1969, Journal of the neurological sciences.