Evaluation of Fanconi Anemia genes in familial breast cancer predisposition
Evaluation of Fanconi Anemia genes in familial breast cancer predisposition
Fanconi Anemia (FA) is an autosomal recessive syndrome characterized by congenital abnormalities, progressive bone marrow failure, and susceptibility to cancer. FA has eight known complementation groups and is caused by mutations in at least seven genes. Biallelic BRCA2 mutations were shown recently to cause FA-D1. Monoallelic (heterozygous) BRCA2 mutations confer a high risk of breast cancer and are a major cause of familial breast cancer. To investigate whether heterozygous variants in other FA genes are high penetrance breast cancer susceptibility alleles, we screened germ-line DNA from 88 BRCA1/2-negative families, each with at least three cases of breast cancer, for mutations in FANCA, FANCC, FANCD2, FANCE, FANCF, and FANCG. Sixty-nine sequence variants were identified of which 25 were exonic. None of the exonic variants resulted in translational frameshifts or nonsense codons and 14 were polymorphisms documented previously. Of the remaining 11 exonic variants, 2 resulted in synonymous changes, and 7 were present in controls. Only 2 conservative missense variants, 1 in FANCA and 1 in FANCE, were each found in a single family and were not present in 300 controls. The results indicate that FA gene mutations, other than in BRCA2, are unlikely to be a frequent cause of highly penetrant breast cancer predisposition.
8596-8599
Seal, Sheila
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Barfoot, Rita
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Jayatilake, Hiran
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Smith, Paula
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Renwick, Anthony
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Bascombe, Linda
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McGuffog, Lesley
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Evans, D. Gareth
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Eccles, Diana
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Easton, Douglas F.
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Stratton, Michael R.
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Rahman, Nazneen
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2003
Seal, Sheila
d8090fdd-aa7a-40c4-a4e4-18a094e7671f
Barfoot, Rita
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Jayatilake, Hiran
fce4b891-57b1-48e7-a276-b77ac5b490bf
Smith, Paula
d32dabeb-91ba-4de4-a968-472fd11567ad
Renwick, Anthony
3d9b9053-ec16-41a7-963d-b72f63c44cc9
Bascombe, Linda
08ee4ea8-8a9b-4171-bc99-adb874215d6c
McGuffog, Lesley
21522096-38bb-45df-aa56-caf2f27d7254
Evans, D. Gareth
314acefb-89fb-4eb7-a0e7-0a6949c9af6c
Eccles, Diana
5b59bc73-11c9-4cf0-a9d5-7a8e523eee23
Easton, Douglas F.
2661cf5e-8fc6-4f1d-b27a-e60cac8c8819
Stratton, Michael R.
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Rahman, Nazneen
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Seal, Sheila, Barfoot, Rita, Jayatilake, Hiran, Smith, Paula, Renwick, Anthony, Bascombe, Linda, McGuffog, Lesley, Evans, D. Gareth, Eccles, Diana, Easton, Douglas F., Stratton, Michael R. and Rahman, Nazneen
(2003)
Evaluation of Fanconi Anemia genes in familial breast cancer predisposition.
Cancer Research, 63 (24), .
Abstract
Fanconi Anemia (FA) is an autosomal recessive syndrome characterized by congenital abnormalities, progressive bone marrow failure, and susceptibility to cancer. FA has eight known complementation groups and is caused by mutations in at least seven genes. Biallelic BRCA2 mutations were shown recently to cause FA-D1. Monoallelic (heterozygous) BRCA2 mutations confer a high risk of breast cancer and are a major cause of familial breast cancer. To investigate whether heterozygous variants in other FA genes are high penetrance breast cancer susceptibility alleles, we screened germ-line DNA from 88 BRCA1/2-negative families, each with at least three cases of breast cancer, for mutations in FANCA, FANCC, FANCD2, FANCE, FANCF, and FANCG. Sixty-nine sequence variants were identified of which 25 were exonic. None of the exonic variants resulted in translational frameshifts or nonsense codons and 14 were polymorphisms documented previously. Of the remaining 11 exonic variants, 2 resulted in synonymous changes, and 7 were present in controls. Only 2 conservative missense variants, 1 in FANCA and 1 in FANCE, were each found in a single family and were not present in 300 controls. The results indicate that FA gene mutations, other than in BRCA2, are unlikely to be a frequent cause of highly penetrant breast cancer predisposition.
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Published date: 2003
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Local EPrints ID: 26599
URI: http://eprints.soton.ac.uk/id/eprint/26599
ISSN: 0008-5472
PURE UUID: 0ba192a9-5c66-43fa-aaef-223ec91e1147
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Date deposited: 20 Apr 2006
Last modified: 23 Jul 2022 01:34
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Contributors
Author:
Sheila Seal
Author:
Rita Barfoot
Author:
Hiran Jayatilake
Author:
Paula Smith
Author:
Anthony Renwick
Author:
Linda Bascombe
Author:
Lesley McGuffog
Author:
D. Gareth Evans
Author:
Douglas F. Easton
Author:
Michael R. Stratton
Author:
Nazneen Rahman
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