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The molecular genetic make-up of male breast cancer

Authors :
Nicolle Besselink
Pier Selenica
Pjotr Prins
Britta Weigelt
Bert van der Vegt
Cathy B. Moelans
Peter Bult
Carmen C. van der Pol
Marco J. Koudijs
Marlous Hoogstraat
Robert Kornegoor
Jorge S. Reis-Filho
Paul J. van Diest
Natalie D. ter Hoeve
Isaac J. Nijman
Elsken van der Wall
Edwin Cuppen
Emile E. Voest
John W.M. Martens
Petra van der Groep
Wendy W.J. de Leng
Joep de Ligt
Miangela M. Lacle
Ellis Barbé
Vincent T.H.B.M. Smit
Pathology
Other Research
Medical Oncology
Damage and Repair in Cancer Development and Cancer Treatment (DARE)
Source :
Endocr Relat Cancer, Endocrine-Related Cancer, 26(10), 779-794. Society for Endocrinology, Endocrine-Related Cancer, 26(10), 779. Society for Endocrinology, Endocrine-Related Cancer, 26(10), 779-794. Bioscientifica Ltd, Endocrine-Related cancer, 26(10), 779-794. BIOSCIENTIFICA LTD, Moelans, C B, de Ligt, J, van der Groep, P, Prins, P, Besselink, N J M, Hoogstraat, M, ter Hoeve, N D, Lacle, M M, Kornegoor, R, van der Pol, C C, de Leng, W W J, Barbé, E, van der Vegt, B, Martens, J, Bult, P, Smit, V T H B M, Koudijs, M J, Nijman, I J, Voest, E E, Selenica, P, Weigelt, B, Reis-Filho, J S, van der Wall, E, Cuppen, E & van Diest, P J 2019, ' The molecular genetic make-up of male breast cancer ', Endocrine-Related Cancer, vol. 26, no. 10, pp. 779-794 . https://doi.org/10.1530/ERC-19-0278
Publication Year :
2019
Publisher :
Bioscientifica, 2019.

Abstract

Male breast cancer (MBC) is extremely rare and accounts for less than 1% of all breast malignancies. Therefore, clinical management of MBC is currently guided by research on the disease in females. In this study, DNA obtained from 45 formalin-fixed paraffin-embedded (FFPE) MBCs with and 90 MBCs (52 FFPE and 38 fresh-frozen) without matched normal tissues was subjected to massively parallel sequencing targeting all exons of 1943 cancer-related genes. The landscape of mutations and copy number alterations was compared to that of publicly available estrogen receptor (ER)-positive female breast cancers (smFBCs) and correlated to prognosis. From the 135 MBCs, 90% showed ductal histology, 96% were ER-positive, 66% were progesterone receptor (PR)-positive, and 2% HER2-positive, resulting in 50, 46 and 4% luminal A-like, luminal B-like and basal-like cases, respectively. Five patients had Klinefelter syndrome (4%) and 11% of patients harbored pathogenic BRCA2 germline mutations. The genomic landscape of MBC to some extent recapitulated that of smFBC, with recurrent PIK3CA (36%) and GATA3 (15%) somatic mutations, and with 40% of the most frequently amplified genes overlapping between both sexes. TP53 (3%) somatic mutations were significantly less frequent in MBC compared to smFBC, whereas somatic mutations in genes regulating chromatin function and homologous recombination deficiency-related signatures were more prevalent. MDM2 amplifications were frequent (13%), correlated with protein overexpression (P = 0.001) and predicted poor outcome (P = 0.007). In conclusion, despite similarities in the genomic landscape between MBC and smFBC, MBC is a molecularly unique and heterogeneous disease requiring its own clinical trials and treatment guidelines.

Details

ISSN :
14796821 and 13510088
Volume :
26
Database :
OpenAIRE
Journal :
Endocrine-Related Cancer
Accession number :
edsair.doi.dedup.....6aa6b4a6b68e01d6ead9ec5f26ffcec3
Full Text :
https://doi.org/10.1530/erc-19-0278