Haplotype and phenotype analysis of six recurrent BRCA1 mutations in 61 families: results of an international study. |
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| Authors: | S. L. Neuhausen S. Mazoyer L. Friedman M. Stratton K. Offit A. Caligo G. Tomlinson L. Cannon-Albright T. Bishop D. Kelsell E. Solomon B. Weber F. Couch J. Struewing P. Tonin F. Durocher S. Narod M. H. Skolnick G. Lenoir O. Serova B. Ponder D. Stoppa-Lyonnet D. Easton M. C. King D. E. Goldgar |
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| Affiliation: | Department of Medical Informatics, University of Utah School of Medicine, Salt Lake City 84108, USA. |
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| Abstract: | Several BRCA1 mutations have now been found to occur in geographically diverse breast and ovarian cancer families. To investigate mutation origin and mutation-specific phenotypes due to BRCA1, we constructed a haplotype of nine polymorphic markers within or immediately flanking the BRCA1 locus in a set of 61 breast/ovarian cancer families selected for having one of six recurrent BRCA1 mutations. Tests of both mutations and family-specific differences in age at diagnosis were not significant. A comparison of the six mutations in the relative proportions of cases of breast and ovarian cancer was suggestive of an effect (P = .069), with 57% of women presumed affected because of the 1294 del 40 BRCA1 mutation having ovarian cancer, compared with 14% of affected women with the splice-site mutation in intron 5 of BRCA1. For the BRCA1 mutations studied here, the individual mutations are estimated to have arisen 9-170 generations ago. In general, a high degree of haplotype conservation across the region was observed, with haplotype differences most often due to mutations in the short-tandem-repeat markers, although some likely instances of recombination also were observed. For several of the instances, there was evidence for multiple, independent, BRCA1 mutational events. |
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