Somatic Mutational Profile of High-Grade Serous Ovarian Carcinoma and Triple-Negative Breast Carcinoma in Young and Elderly Patients: Similarities and Divergences

Pedro Adolpho de Menezes Pacheco Serio; Gláucia Fernanda de Lima Pereira; Maria Lucia Hirata Katayama; Rosimeire Aparecida Roela; Simone Maistro; Maria Aparecida Azevedo Koike Folgueira

doi:10.3390/cells10123586

Somatic Mutational Profile of High-Grade Serous Ovarian Carcinoma and Triple-Negative Breast Carcinoma in Young and Elderly Patients: Similarities and Divergences

Cells. 2021 Dec 20;10(12):3586. doi: 10.3390/cells10123586.

Authors

Pedro Adolpho de Menezes Pacheco Serio¹, Gláucia Fernanda de Lima Pereira¹, Maria Lucia Hirata Katayama¹, Rosimeire Aparecida Roela¹, Simone Maistro¹, Maria Aparecida Azevedo Koike Folgueira¹

Affiliation

¹ Centro de Investigação Translacional em Oncologia, Departamento de Radiologia e Oncologia, Instituto do Cancer do Estado de Sao Paulo, Hospital das Clinicas HCFMUSP, Faculdade de Medicina, Universidade de Sao Paulo, Sao Paulo 01246-000, Brazil.

Abstract

Background: Triple-negative breast cancer (TNBC) and High-Grade Serous Ovarian Cancer (HGSOC) are aggressive malignancies that share similarities; however, different ages of onset may reflect distinct tumor behaviors. Thus, our aim was to compare somatic mutations in potential driver genes in 109 TNBC and 81 HGSOC from young (Y ≤ 40 years) and elderly (E ≥ 75 years) patients.

Methods: Open access mutational data (WGS or WES) were collected for TNBC and HGSOC patients. Potential driver genes were those that were present in the Cancer Gene Census-CGC, the Candidate Cancer Gene Database-CCGD, or OncoKB and those that were considered pathogenic in variant effect prediction tools.

Results: Mutational signature 3 (homologous repair defects) was the only gene that was represented in all four subgroups. The median number of mutated CGCs per sample was similar in HGSOC (Y:3 vs. E:4), but it was higher in elderly TNBC than it was in young TNBC (Y:3 vs. E:6). At least 90% of the samples from TNBC and HGSOC from Y and E patients presented at least one known affected TSG. Besides TP53, which was mutated in 67-83% of the samples, the affected TSG in TP53 wild-type samples were NF1 (yHGSOC and yTNBC), PHF6 (eHGSOC and yTNBC), PTEN, PIK3R1 and ZHFX3 (yTNBC), KMT2C, ARID1B, TBX3, and ATM (eTNBC). A few samples only presented one affected oncogene (but no TSG): KRAS and TSHR in eHGSOC and RAC1 and PREX2 (a regulator of RAC1) in yTNBC. At least ⅔ of the tumors presented mutated oncogenes associated with tumor suppressor genes; the Ras and/or PIK3CA signaling pathways were altered in 15% HGSOC and 20-35% TNBC (Y vs. E); DNA repair genes were mutated in 19-33% of the HGSOC tumors but were more frequently mutated in E-TNBC (56%). However, in HGSOC, 9.5% and 3.3% of the young and elderly patients, respectively, did not present any tumors with an affected CGC nor did 4.65% and none of the young and elderly TNBC patients.

Conclusion: Most HGSOC and TNBC from young and elderly patients present an affected TSG, mainly TP53, as well as mutational signature 3; however, a few tumors only present an affected oncogene or no affected cancer-causing genes.

Keywords: high-grade serous ovarian carcinoma; somatic; triple-negative breast cancer; young adult.

MeSH terms

Adult
Aged
Cystadenocarcinoma, Serous / genetics*
Cystadenocarcinoma, Serous / pathology*
DNA Mutational Analysis
DNA Repair / genetics
Female
Genes, Tumor Suppressor
Genetic Variation
Humans
Mutation / genetics*
Neoplasm Grading
Oncogenes
Ovarian Neoplasms / genetics*
Ovarian Neoplasms / pathology*
Triple Negative Breast Neoplasms / genetics*