The mutational landscape of a US Midwestern breast cancer cohort reveals subtype-specific cancer drivers and prognostic markers

Neetha Nanoth Vellichirammal; Yuan-De Tan; Peng Xiao; James Eudy; Oleg Shats; David Kelly; Michelle Desler; Kenneth Cowan; Chittibabu Guda

doi:10.1186/s40246-023-00511-6

The mutational landscape of a US Midwestern breast cancer cohort reveals subtype-specific cancer drivers and prognostic markers

Hum Genomics. 2023 Jul 15;17(1):64. doi: 10.1186/s40246-023-00511-6.

Authors

Neetha Nanoth Vellichirammal¹, Yuan-De Tan¹, Peng Xiao¹, James Eudy¹, Oleg Shats^{2

3}, David Kelly^{2

3}, Michelle Desler^{2

3}, Kenneth Cowan^{2

3}, Chittibabu Guda^{4

5

6}

Affiliations

¹ Department of Genetics, Cell Biology and Anatomy, University of Nebraska Medical Center, Omaha, NE, 68198, USA.
² Eppley Institute for Research in Cancer and Allied Diseases, University of Nebraska Medical Center, Omaha, NE, USA.
³ Fred and Pamela Buffett Cancer Center, University of Nebraska Medical Center, Omaha, USA.
⁴ Department of Genetics, Cell Biology and Anatomy, University of Nebraska Medical Center, Omaha, NE, 68198, USA. babu.guda@unmc.edu.
⁵ Center for Biomedical Informatics Research and Innovation, University of Nebraska Medical Center, Omaha, NE, 68198, USA. babu.guda@unmc.edu.
⁶ Fred and Pamela Buffett Cancer Center, University of Nebraska Medical Center, Omaha, USA. babu.guda@unmc.edu.

Abstract

Background: Female breast cancer remains the second leading cause of cancer-related death in the USA. The heterogeneity in the tumor morphology across the cohort and within patients can lead to unpredictable therapy resistance, metastasis, and clinical outcome. Hence, supplementing classic pathological markers with intrinsic tumor molecular markers can help identify novel molecular subtypes and the discovery of actionable biomarkers.

Methods: We conducted a large multi-institutional genomic analysis of paired normal and tumor samples from breast cancer patients to profile the complex genomic architecture of breast tumors. Long-term patient follow-up, therapeutic regimens, and treatment response for this cohort are documented using the Breast Cancer Collaborative Registry. The majority of the patients in this study were at tumor stage 1 (51.4%) and stage 2 (36.3%) at the time of diagnosis. Whole-exome sequencing data from 554 patients were used for mutational profiling and identifying cancer drivers.

Results: We identified 54 tumors having at least 1000 mutations and 185 tumors with less than 100 mutations. Tumor mutational burden varied across the classified subtypes, and the top ten mutated genes include MUC4, MUC16, PIK3CA, TTN, TP53, NBPF10, NBPF1, CDC27, AHNAK2, and MUC2. Patients were classified based on seven biological and tumor-specific parameters, including grade, stage, hormone receptor status, histological subtype, Ki67 expression, lymph node status, race, and mutational profiles compared across different subtypes. Mutual exclusion of mutations in PIK3CA and TP53 was pronounced across different tumor grades. Cancer drivers specific to each subtype include TP53, PIK3CA, CDC27, CDH1, STK39, CBFB, MAP3K1, and GATA3, and mutations associated with patient survival were identified in our cohort.

Conclusions: This extensive study has revealed tumor burden, driver genes, co-occurrence, mutual exclusivity, and survival effects of mutations on a US Midwestern breast cancer cohort, paving the way for developing personalized therapeutic strategies.

MeSH terms

Biomarkers, Tumor / genetics
Breast Neoplasms* / genetics
Breast Neoplasms* / pathology
Class I Phosphatidylinositol 3-Kinases / genetics
Female
Humans
Mutation
Prognosis

Substances

Biomarkers, Tumor
Class I Phosphatidylinositol 3-Kinases

Abstract

MeSH terms

Substances

Grants and funding