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Surveillance for familial breast cancer: differences in outcome according to BRCA mutation status

Surveillance for familial breast cancer: differences in outcome according to BRCA mutation status
Surveillance for familial breast cancer: differences in outcome according to BRCA mutation status
Women with a family history of breast cancer are commonly offered regular clinical or mammographic surveillance from age 30. Data on the efficacy of such programmes are limited. Clinical, pathological and outcome data were recorded on all breast and ovarian cancers diagnosed within familial breast cancer surveillance programmes at collaborating centers in Norway and the UK up to the end of 2005. These have been analyzed according to the mutation status of the affected women (BRCAI+ve, BRCA2+ve or mutation-negative). Breast cancer was diagnosed in 442 patients subsequently followed for a total of 2095 years. Eightynine (20%) had BRCA1 mutations, 35 (8%) BRCA2 mutations and in 318 (72%) no mutation could be detected ("mut neg"). Fiveyear survival in BRCA1 was 73% compared to 96% in BRCA2 and 92% in mut neg (p = 0.000). Among BRCA1 mutation-carriers, 5-year survival was 67% for cases diagnosed as carcinoma in situ, 84% for node-negative invasive cancers and 58% for those with nodal involvement (p > 0.05). For BRCA2 mutation-carriers the corresponding figures were 100, 100 and 90% (p > 0.05), while for mut neg women they were 100, 97 and 71 % (p = 0.03). Regular surveillance in women at increased familial risk of breast cancer is associated with a good outcome if they carry BRCA2 mutations or no detectable mutation. Carriers of BRCA1 mutations fare significantly worse, even when their tumors are diagnosed at an apparently early stage. The differences in outcome associated with different genetic causes of disease were associated with demonstrated differences in tumor biology. The findings demonstrate the outcome for genetically different breast cancers detected within a programme for early diagnosis and treatment, wh ch is relevant to genetic counseling when women at risk have to chose between the options for preventing death from inherited breast cancer. (C) 2007 Wiley-Liss, Inc
BRCA1, BRCA2, breast cancer, inherited, outcome, prospective trail, early diagnosis
0020-7136
1017-1020
Moller, Pal
72f197e1-cd66-4f9e-863f-f671ac8670c2
Evans, D. Gareth
314acefb-89fb-4eb7-a0e7-0a6949c9af6c
Reis, Marta M.
936d476d-5a74-4beb-9e10-8c4ac2d8efd9
Gregory, Helen
d486c9b1-6c6c-4cc1-9240-9e2c7db5495e
Anderson, Elaine
08c77229-6c2b-48c7-b723-c2b5b258a5f1
Maehle, Lovise
d36d3d47-c751-4744-bc73-d82fd6bf47d4
Lalloo, Fiona
d7ac29ee-10db-49a5-af3c-265b6d1c113d
Howell, Anthony
1a0a7e78-3d51-4e76-8cd5-bd46cb90d588
Apold, Jaran
39f4a511-7b54-44a1-a7cb-1b3924eca9a8
Clark, Neal
207b15b1-73ff-4549-957e-460e46bdb354
Lucassen, Anneke
2eb85efc-c6e8-4c3f-b963-0290f6c038a5
Steel, C. Michael
a68bafc7-571b-4deb-b763-3ec5c8073808
Moller, Pal
72f197e1-cd66-4f9e-863f-f671ac8670c2
Evans, D. Gareth
314acefb-89fb-4eb7-a0e7-0a6949c9af6c
Reis, Marta M.
936d476d-5a74-4beb-9e10-8c4ac2d8efd9
Gregory, Helen
d486c9b1-6c6c-4cc1-9240-9e2c7db5495e
Anderson, Elaine
08c77229-6c2b-48c7-b723-c2b5b258a5f1
Maehle, Lovise
d36d3d47-c751-4744-bc73-d82fd6bf47d4
Lalloo, Fiona
d7ac29ee-10db-49a5-af3c-265b6d1c113d
Howell, Anthony
1a0a7e78-3d51-4e76-8cd5-bd46cb90d588
Apold, Jaran
39f4a511-7b54-44a1-a7cb-1b3924eca9a8
Clark, Neal
207b15b1-73ff-4549-957e-460e46bdb354
Lucassen, Anneke
2eb85efc-c6e8-4c3f-b963-0290f6c038a5
Steel, C. Michael
a68bafc7-571b-4deb-b763-3ec5c8073808

Moller, Pal, Evans, D. Gareth, Reis, Marta M., Gregory, Helen, Anderson, Elaine, Maehle, Lovise, Lalloo, Fiona, Howell, Anthony, Apold, Jaran, Clark, Neal, Lucassen, Anneke and Steel, C. Michael (2007) Surveillance for familial breast cancer: differences in outcome according to BRCA mutation status. International Journal of Cancer, 121 (5), 1017-1020. (doi:10.1002/ijc.22789).

Record type: Article

Abstract

Women with a family history of breast cancer are commonly offered regular clinical or mammographic surveillance from age 30. Data on the efficacy of such programmes are limited. Clinical, pathological and outcome data were recorded on all breast and ovarian cancers diagnosed within familial breast cancer surveillance programmes at collaborating centers in Norway and the UK up to the end of 2005. These have been analyzed according to the mutation status of the affected women (BRCAI+ve, BRCA2+ve or mutation-negative). Breast cancer was diagnosed in 442 patients subsequently followed for a total of 2095 years. Eightynine (20%) had BRCA1 mutations, 35 (8%) BRCA2 mutations and in 318 (72%) no mutation could be detected ("mut neg"). Fiveyear survival in BRCA1 was 73% compared to 96% in BRCA2 and 92% in mut neg (p = 0.000). Among BRCA1 mutation-carriers, 5-year survival was 67% for cases diagnosed as carcinoma in situ, 84% for node-negative invasive cancers and 58% for those with nodal involvement (p > 0.05). For BRCA2 mutation-carriers the corresponding figures were 100, 100 and 90% (p > 0.05), while for mut neg women they were 100, 97 and 71 % (p = 0.03). Regular surveillance in women at increased familial risk of breast cancer is associated with a good outcome if they carry BRCA2 mutations or no detectable mutation. Carriers of BRCA1 mutations fare significantly worse, even when their tumors are diagnosed at an apparently early stage. The differences in outcome associated with different genetic causes of disease were associated with demonstrated differences in tumor biology. The findings demonstrate the outcome for genetically different breast cancers detected within a programme for early diagnosis and treatment, wh ch is relevant to genetic counseling when women at risk have to chose between the options for preventing death from inherited breast cancer. (C) 2007 Wiley-Liss, Inc

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Published date: 30 April 2007
Related URLs:
Keywords: BRCA1, BRCA2, breast cancer, inherited, outcome, prospective trail, early diagnosis

Identifiers

Local EPrints ID: 62854
URI: http://eprints.soton.ac.uk/id/eprint/62854
DOI: doi:10.1002/ijc.22789
ISSN: 0020-7136
PURE UUID: 7fd4e49c-2d7f-4c13-a43f-525ae1b8a805
ORCID for Anneke Lucassen: ORCID iD orcid.org/0000-0003-3324-4338

Catalogue record

Date deposited: 05 Sep 2008
Last modified: 16 Mar 2024 03:23

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Contributors

Author: Pal Moller
Author: D. Gareth Evans
Author: Marta M. Reis
Author: Helen Gregory
Author: Elaine Anderson
Author: Lovise Maehle
Author: Fiona Lalloo
Author: Anthony Howell
Author: Jaran Apold
Author: Neal Clark
Author: Anneke Lucassen ORCID iD
Author: C. Michael Steel

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