Population-specific Mutation Patterns in Breast Tumors from African American, European American, and Kenyan Patients

Author:

Tang Wei12ORCID,Zhang Flora13ORCID,Byun Jung S.4ORCID,Dorsey Tiffany H.1ORCID,Yfantis Harris G.5ORCID,Ajao Anuoluwapo1ORCID,Liu Huaitian1ORCID,Pichardo Margaret S.16ORCID,Pichardo Catherine M.17ORCID,Harris Alexandra R.18ORCID,Yang Xiaohong R.8ORCID,Figueroa Jonine D.8ORCID,Sayed Shahin9ORCID,Makokha Francis W.10ORCID,Ambs Stefan1ORCID

Affiliation:

1. 1Laboratory of Human Carcinogenesis, Center for Cancer Research, NCI, NIH, Bethesda, Maryland.

2. 2Data Science & Artificial Intelligence, R&D, AstraZeneca, Gaithersburg, Maryland.

3. 3Colgate University, Hamilton, New York.

4. 4Division of Intramural Research, National Institute of Minority Health and Health Disparities, NIH, Bethesda, Maryland.

5. 5Department of Pathology, University of Maryland Medical Center and Veterans Affairs, Maryland Care System, Baltimore, Maryland.

6. 6Department of Surgery, Hospital of the University of Pennsylvania, Penn Medicine, Philadelphia, Pennsylvania.

7. 7Division of Cancer Control and Population Sciences, NCI, NIH, Rockville, Maryland.

8. 8Integrative Tumor Epidemiology Branch, Division of Cancer Epidemiology and Genetics, NCI, Rockville, Maryland.

9. 9Aga Khan University Hospital, Nairobi, Kenya.

10. 10Mount Kenya University, Thika, Kenya.

Abstract

Abstract Women of African descent have the highest breast cancer mortality in the United States and are more likely than women from other population groups to develop an aggressive disease. It remains uncertain to what extent breast cancer in Africa is reminiscent of breast cancer in African American or European American patients. Here, we performed whole-exome sequencing of genomic DNA from 191 breast tumor and non-cancerous adjacent tissue pairs obtained from 97 African American, 69 European American, 2 Asian American, and 23 Kenyan patients. Our analysis of the sequencing data revealed an elevated tumor mutational burden in both Kenyan and African American patients, when compared with European American patients. TP53 mutations were most prevalent, particularly in African American patients, followed by PIK3CA mutations, which showed similar frequencies in European American, African American, and the Kenyan patients. Mutations targeting TBX3 were confined to European Americans and those targeting the FBXW7 tumor suppressor to African American patients whereas mutations in the ARID1A gene that are known to confer resistance to endocrine therapy were distinctively enriched among Kenyan patients. A Kyoto Encyclopedia of Genes and Genomes pathway analysis could link FBXW7 mutations to an increased mitochondrial oxidative phosphorylation capacity in tumors carrying these mutations. Finally, Catalogue of Somatic Mutations in Cancer (COSMIC) mutational signatures in tumors correlated with the occurrence of driver mutations, immune cell profiles, and neighborhood deprivation with associations ranging from being mostly modest to occasionally robust. To conclude, we found mutational profiles that were different between these patient groups. The differences concentrated among genes with low mutation frequencies in breast cancer. Significance: The study describes differences in tumor mutational profiles between African American, European American, and Kenyan breast cancer patients. It also investigates how these profiles may relate to the tumor immune environment and the neighborhood environment in which the patients had residence. Finally, it describes an overrepresentation of ARID1A gene mutations in breast tumors of the Kenyan patients.

Funder

HHS | NIH | National Cancer Institute

National Research Fund, Kenya

HHS | NIH | National Institute on Minority Health and Health Disparities

Publisher

American Association for Cancer Research (AACR)

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