Population Differences in Breast Cancer: Survey in Indigenous African Women Reveals Over-Representation of Triple-Negative Breast Cancer

Author:

Huo Dezheng1,Ikpatt Francis1,Khramtsov Andrey1,Dangou Jean-Marie1,Nanda Rita1,Dignam James1,Zhang Bifeng1,Grushko Tatyana1,Zhang Chunling1,Oluwasola Olayiwola1,Malaka David1,Malami Sani1,Odetunde Abayomi1,Adeoye Adewumi O.1,Iyare Festus1,Falusi Adeyinka1,Perou Charles M.1,Olopade Olufunmilayo I.1

Affiliation:

1. From the Department of Health Studies, and Section of Hematology/Oncology, Department of Medicine, University of Chicago, Chicago, IL; Institut Pasteur, Dakar, Sénégal; University of Ibadan, Ibadan; Usman Danfodio University Teaching Hospital, Sokoto; Ebonyi State University Teaching Hospital, Abakaliki, Nigeria; and University of North Carolina, Chapel Hill, NC.

Abstract

Purpose Compared with white women, black women experience a disproportionate burden of aggressive breast cancer for reasons that remain unknown and understudied. In the first study of its kind, we determined the distribution of molecular subtypes of invasive breast tumors in indigenous black women in West Africa. Patients and Methods The study comprised 507 patients diagnosed with breast cancer between 1996 and 2007 at six geographic regions in Nigeria and Senegal. Formalin-fixed and paraffin-embedded sections were constructed into tissue microarrays and immunostained with 15 antibodies. Five molecular subtypes were determined, and hierarchical cluster analysis was conducted to explore subgroups for unclassified cases. Results The mean (± standard deviation) age of 378 patients in the first cohort was 44.8 ± 11.8 years, with the majority of women presenting with large (4.4 ± 2.0 cm) high-grade tumors (83%) in advanced stages (72% node positive). The proportions of estrogen receptor (ER) –positive, progesterone receptor–positive, and human epidermal growth factor receptor 2 (HER2) –positive tumors were 24%, 20%, and 17%, respectively. Triple negativity for these markers was predominant, including basal-like (27%) and unclassified subtype (28%). Other subtypes were luminal A (27%), luminal B (2%), and HER2 positive/ER negative (15%). The findings were replicated in the second cohort of 129 patients. The unclassified cases could be grouped into a bad prognosis branch, with expression of vascular endothelial growth factor, B-cell lymphoma extra-large protein, and Cyclin E, and a good prognosis branch, with expression of B-cell lymphoma protein 2 and Cyclin D1. Conclusion These findings underscore the urgent need for research into the etiology and treatment of the aggressive molecular subtypes that disproportionately affect young women in the African diaspora.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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