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BRCA1 Genomic Deletions Are Major Founder Mutations in Dutch Breast Cancer Patients

Overview
Journal Nat Genet
Specialty Genetics
Date 1997 Nov 14
PMID 9354803
Citations 102
Authors
T Peelen
M van Vliet
R van Eijk
R Olmer
M Drusedau
F B Hogervorst
S Hageman
P J Arts
M J Ligtenberg
H Meijers-Heijboer
J G Klijn
H F Vasen
C J Cornelisse
L J van t Veer
E Bakker
G J van Ommen
P Devilee
Affiliations
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Abstract

To date, more than 300 distinct small deletions, insertions and point mutations, mostly leading to premature termination of translation, have been reported in the breast/ovarian-cancer susceptibility gene BRCA1. The elevated frequencies of some mutations in certain ethnic subpopulations are caused by founder effects, rather than by mutation hotspots. Here we report that the currently available mutation spectrum of BRCA1 has been biased by PCR-based mutation-screening methods, such as SSCP, the protein truncation test (PTT) and direct sequencing, using genomic DNA as template. Three large genomic deletions that are not detected by these approaches comprise 36% of all BRCA1 mutations found in Dutch breast-cancer families to date. A 510-bp Alu-mediated deletion comprising exon 22 was found in 8 of 170 breast-cancer families recruited for research purposes and in 6 of 49 probands referred to the Amsterdam Family Cancer Clinic for genetic counselling. In addition, a 3,835-bp Alu-mediated deletion encompassing exon 13 was detected in 4 of 170 research families, while an deletion of approximately 14 kb was detected in a single family [corrected]. Haplotype analyses indicated that each recurrent deletion had a single common ancestor.

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