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      Spectrum and frequencies of BRCA1/2 mutations in Bulgarian high risk breast cancer patients

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          Abstract

          Background

          About 3885 women are diagnosed with breast cancer and 1285 die from the disease each year in Bulgaria. However no genetic testing to identify the mutations in high-risk families has been provided so far.

          Methods

          We evaluated 200 Bulgarian women with primary invasive breast cancer and with personal/ family history of breast cancer for the presence of unequivocally damaging germline mutations in BRCA1/2 using Sanger sequencing.

          Results

          Of the 200 patients, 39 (19.5 %) carried a disease predisposing mutation, including 28 (14 %) with a BRCA1 mutation and 11 (5.5 %) with a BRCA2 mutation. At BRCA1, 6 different mutations were identified, including 2 frameshifts, 1 nonsense and 1 missense that had been previously reported (c.5030_5033delCTAA, c.5263_5264insC, c.4603G > T, c.181 T > G), and 2 frameshifts, which were novel to this study (c.464delA, c.5397_5403delCCCTTGG). At BRCA2, 7 different frameshift mutations were identified, including 5 previously reported (5851_5854delAGTT, c.5946delT, c.5718_5719delCT, c.7910_7914delCCTTT,c.9098_9099insA) and 2 novel (c.8532_8533delAA, c.9682delA).

          A BRCA1 mutation was found in 18.4 % of women diagnosed with breast cancer at/or under the age of 40 compared to 11.2 % of women diagnosed at a later age; a BRCA2 mutation was found in 4 % of women diagnosed at/or under the age of 40 compared to 6.5 % of women diagnosed at a later age. A mutation was present in 26.8 % patients with a positive family history and in 14.4 % of women with a negative family history.

          The most prevalent mutation observed in 22 patients (11 %) was BRCA1 c.5263_5264insC, a known Slavic mutation with founder effect in Eastern European and AJ communities. Other recurrent mutations were BRCA2 c.9098-9099insA (2 %), BRCA1 c.181T > G (1 %) and BRCA2 c.5851_5854delAGTT (1 %). Notably, BRCA1 c.5263_5264insC represented 56 % of all mutations identified in this series. Of the 22 patients with BRCA1 c.5263_5264insC, 9 were diagnosed with early onset breast cancer, 11 with TNBCs, 4 with bilateral breast cancer, and 6 with both breast and ovarian cancer.

          Conclusions

          This is the first comprehensive study of the BRCA1/2 mutation spectrum in Bulgaria and will assist the establishment of efficient protocols for genetic testing and individualized risk assessment for Bulgarian breast/ovarian cancer patients and healthy individuals at a high-risk.

          Electronic supplementary material

          The online version of this article (doi:10.1186/s12885-015-1516-2) contains supplementary material, which is available to authorized users.

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          Most cited references31

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          A strong candidate for the breast and ovarian cancer susceptibility gene BRCA1.

          Y Miki, J. Swensen, D Shattuck-Eidens (1994)
          A strong candidate for the 17q-linked BRCA1 gene, which influences susceptibility to breast and ovarian cancer, has been identified by positional cloning methods. Probable predisposing mutations have been detected in five of eight kindreds presumed to segregate BRCA1 susceptibility alleles. The mutations include an 11-base pair deletion, a 1-base pair insertion, a stop codon, a missense substitution, and an inferred regulatory mutation. The BRCA1 gene is expressed in numerous tissues, including breast and ovary, and encodes a predicted protein of 1863 amino acids. This protein contains a zinc finger domain in its amino-terminal region, but is otherwise unrelated to previously described proteins. Identification of BRCA1 should facilitate early diagnosis of breast and ovarian cancer susceptibility in some individuals as well as a better understanding of breast cancer biology.
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            Cancer risks in BRCA2 mutation carriers.

            (1999)
            Carriers of germline mutations in the BRCA2 gene are known to be at high risk of breast and ovarian cancers, but the risks of other cancers in mutation carriers are uncertain. We investigated these risks in 173 breast-ovarian cancer families with BRCA2 mutations identified at 20 centers in Europe and North America. Other cancer occurrence was determined in a final cohort of 3728 individuals, among whom 681 persons had breast or ovarian cancer and 3047 persons either were known mutation carriers, were first-degree relatives of known mutation carriers, or were first-degree relatives of breast or ovarian cancer patients. Incidence rates were compared with population-specific incidence rates, and relative risks (RRs) to carriers, together with 95% confidence intervals (CIs), were estimated by use of a maximum likelihood approach. Three hundred thirty-three other cancers occurred in this cohort. Statistically significant increases in risks were observed for prostate cancer (estimated RR = 4.65; 95% CI = 3.48-6.22), pancreatic cancer (RR = 3.51; 95% CI = 1. 87-6.58), gallbladder and bile duct cancer (RR = 4.97; 95% CI = 1. 50-16.52), stomach cancer (RR = 2.59; 95%CI = 1.46-4.61), and malignant melanoma (RR = 2.58; 95% CI = 1.28-5.17). The RR for prostate cancer for men below the age of 65 years was 7.33 (95% CI = 4.66-11.52). Among women who had already developed breast cancer, the cumulative risks of a second, contralateral breast cancer and of ovarian cancer by the age of 70 years were estimated to be 52.3% (95% CI = 41.7%-61.0%) and 15.9% (95% CI = 8.8%-22.5%), respectively. In addition to the large risks of breast and ovarian cancers, BRCA2 mutations may be associated with increased risks of several other cancers.
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              Triple-negative breast cancer: BRCAness and concordance of clinical features with BRCA1-mutation carriers

              E Lips, R L Mulder, A Oonk (2013)
              Background: BRCAness is defined as shared tumour characteristics between sporadic and BRCA-mutated cancers. However, how to exactly measure BRCAness and its frequency in breast cancer is not known. Assays to establish BRCAness would be extremely valuable for the clinical management of these tumours. We assessed BRCAness characteristics frequencies in a large cohort of triple-negative breast cancers (TNBCs). Methods: As a measure of BRCAness, we determined a specific BRCA1-like pattern by array Comparative Genomic Hybridisation (aCGH), and BRCA1 promoter methylation in 377 TNBCs, obtained from 3 different patient cohorts. Clinicopathological data were available for all tumours, BRCA1-germline mutation status and chemotherapy response data were available for a subset. Results: Of the tumours, 66–69% had a BRCA1-like aCGH profile and 27–37% showed BRCA1 promoter methylation. BRCA1-germline mutations and BRCA1 promoter methylation were mutually exclusive events (P=1 × 10−5). BRCAness was associated with younger age and grade 3 tumours. Chemotherapy response was significantly higher in BRCA1-mutated tumours, but not in tumours with BRCAness (63% (12 out of 19) vs 35% (18 out of 52) pathological complete remission rate, respectively). Conclusion: The majority of the TNBCs show BRCAness, and those tumours share clinicopathological characteristics with BRCA1-mutated tumours. A better characterisation of TNBC and the presence of BRCAness could have consequences for both hereditary breast cancer screening and the treatment of these tumours.
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                Author and article information

                Contributors
                Rumyana Ivanova Dodova: r.dodova@mmcbg.org
                Atanaska Velichkova Mitkova: +359 2 9172 214 , mitkova@mmcbg.org
                Daniela Rosenova Dacheva: dacheva@mmcbg.org
                Lina Basam Hadjo: linahadjo@yahoo.com
                Alexandrina Ivanova Vlahova: alexandrina_vlahova@yahoo.com
                Margarita Stoyanova Taushanova - Hadjieva: md_margarita@yahoo.com
                Spartak Stoyanov Valev: valev.md@gmail.com
                Marija Mitko Caulevska: caulevska@yahoo.com
                Stanislava Dimitrova Popova: stasi_popova@abv.bg
                Ivan Emilov Popov: thema3xman@googlemail.com
                Tihomir Iliichev Dikov: tih.dikov@abv.bg
                Theophil Angelov Sedloev: theosed@abv.bg
                Atanas Stefanov Ionkov: aionkov@abv.bg
                Konstanta Velinova Timcheva: const_timcheva@hotmail.com
                Svetlana Liubomirova Christova: dr_svetlahristova@yahoo.com
                Ivo Marinov Kremensky: kremensk@yahoo.com
                Vanio Ivanov Mitev: mitev@medfac.acad.bg
                Radka Petrova Kaneva: kaneva@mmcbg.org
                Journal
                Journal ID (nlm-ta): BMC Cancer
                Journal ID (iso-abbrev): BMC Cancer
                Title: BMC Cancer
                Publisher: BioMed Central (London )
                ISSN (Electronic): 1471-2407
                Publication date (Electronic): 17 July 2015
                Publication date PMC-release: 17 July 2015
                Publication date Collection: 2015
                Volume: 15
                Electronic Location Identifier: 523
                Affiliations
                [ ]Molecular Medicine Center, Medical University of Sofia, 2 Zdrave str., 1431 Sofia, Bulgaria
                [ ]Department of Medical Chemistry and Biochemistry, Medical Faculty, Medical University of Sofia, 2 Zdrave str., 1431 Sofia, Bulgaria
                [ ]General and Clinical Pathology Clinic, University Hospital “Alexandrovska”, 1 Georgi Sofiiski str., 1431 Sofia, Bulgaria
                [ ]Department of General and Clinical Pathology, Medical University of Sofia, 1 Georgi Sofiiski str., 1431 Sofia, Bulgaria
                [ ]Clinic of Medical Oncology (Chemotherapy), Specialized Hospital for Active Treatment in Oncology, 6 “Plovdivsko pole” str., 1756 Sofia, Bulgaria
                [ ]Department of Surgery, University Hospital “Tsaritsa Yoana - ISUL”, 8 “Byalo more” str., 1527 Sofia, Bulgaria
                [ ]Medical Faculty, 8 “Byalo more” str., 1527 Sofia, Bulgaria
                [ ]Department of General and Liver-Pancreatic Surgery, University Hospital “Alexandrovska”, 1 Georgi Sofiiski str., 1431 Sofia, Bulgaria
                [ ]Medical Faculty, Medical University of Sofia, 1 Georgi Sofiiski str., 1431 Sofia, Bulgaria
                Article
                Publisher ID: 1516
                DOI: 10.1186/s12885-015-1516-2
                PMC ID: 4504066
                PubMed ID: 26183948
                SO-VID: 3e5271d1-edfb-480c-b16b-5a14d027390a
                Copyright © © Dodova et al. 2015
                License:

                This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver ( http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

                History
                Date received : 4 April 2014
                Date accepted : 26 June 2015
                Categories
                Subject: Research Article
                Custom metadata
                issue-copyright-statement © The Author(s) 2015

                ScienceOpen disciplines: Oncology & Radiotherapy
                Keywords: brca1,brca2,breast cancer,genetic testing,mutations,sequencing
                Data availability:
                ScienceOpen disciplines: Oncology & Radiotherapy
                Keywords: brca1, brca2, breast cancer, genetic testing, mutations, sequencing

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