Linkage and LOH studies in 19 cylindromatosis families show no evidence of genetic heterogeneity and refine the CYLD locus on chromosome 16q12–q13
M Takahashi, E Rapley, PJ Biggs, SR Lakhani… - Human genetics, 2000 - Springer
M Takahashi, E Rapley, PJ Biggs, SR Lakhani, D Cooke, J Hansen, E Blair, B Hofmann…
Human genetics, 2000•SpringerFamilial cylindromatosis is an autosomal dominant predisposition to multiple neoplasms of
the skin appendages. The susceptibility gene has previously been mapped to chromosome
16q12–q13 and has features of a recessive oncogene/tumour suppressor gene. We have
now evaluated 19 families with this disease by a combination of genetic linkage analysis
and loss of heterozygosity in cylindromas from affected individuals. All 15 informative
families show linkage to this locus, providing no evidence for genetic heterogeneity …
the skin appendages. The susceptibility gene has previously been mapped to chromosome
16q12–q13 and has features of a recessive oncogene/tumour suppressor gene. We have
now evaluated 19 families with this disease by a combination of genetic linkage analysis
and loss of heterozygosity in cylindromas from affected individuals. All 15 informative
families show linkage to this locus, providing no evidence for genetic heterogeneity …
Abstract
Familial cylindromatosis is an autosomal dominant predisposition to multiple neoplasms of the skin appendages. The susceptibility gene has previously been mapped to chromosome 16q12–q13 and has features of a recessive oncogene/tumour suppressor gene. We have now evaluated 19 families with this disease by a combination of genetic linkage analysis and loss of heterozygosity in cylindromas from affected individuals. All 15 informative families show linkage to this locus, providing no evidence for genetic heterogeneity. Recombinant mapping has placed the gene in an interval of approximately 1 Mb. There is no evidence, between families, of haplotype sharing that might be indicative of common founder mutations.
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