PO.PS01.07 · 人群科学

Characterizing BRCA1 and BRCA2 mutations in Cameroonian breast cancer patients: Efforts towards bridging the genomic gap in Africa

编号 3596 展板 14 时间 4/20 02:00–05:00 区域 Section 35 主讲 Kenn Chi Ndi, MD
分会场 Genetic Epidemiology 1: GxE, GWAS, Polygenic Risk Scores, and Post-GWAS
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作者与单位

Kenn Chi Ndi1, Berthe Sabine Esson Mapoko2, Vanessa Mouaye3, Carmen Vanvolkenburgh4, Bonaventure Dzekem4, Paul Ndom2, Dezheng Huo4, Olufunmilayo I. Olopade4

1Medical Oncology, Centre Hospitalier Regional d'Ebolowa, Ebolowa, Cameroon,2Medical Oncology, Faculty of Medicine and Biomedical Sciences, University of Yaounde 1, Yaounde, Cameroon,3Cancer Control Committee, Yaounde, Cameroon,4University of Chicago Medical Center, Chicago, IL

摘要 Abstract

Background: There are profound global inequities cancer genomics research, with publications focusing on cancer genetics from Africa representing only 0.016% of the global total. This genomic underrepresentation creates significant barriers to equitable cancer care and precision medicine for African populations. BRCA1/2 mutations remain critically understudied in these communities, limiting our understanding of hereditary breast cancer patterns. This pioneering study characterizes BRCA1/2 mutations among Cameroonian patients to lay the foundation for future genomic research and address critical knowledge gaps. Methods: This hospital-based study recruited 82 breast cancer patients from 2 major treatment centers in Cameroon, an underserved population with limited access to genetic services. Following pre-test genetic counseling, saliva samples were collected and analyzed using next-generation sequencing for 29 cancer-associated genes. AI was used to improve the clarity of the language of this abstract. Results: Pathogenic mutations were identified in 23 patients (28%), with BRCA1 (15) and BRCA2 (2) accounting for 73.9% of all mutations (18.3% and 2.4% of the total population, respectively). The most frequent BRCA1 mutation was c.4484G>T(p.Arg1495Met) , present in 7 patients (46.7% of BRCA1 mutations, 8.5% of total population), followed by c.5155dup(p.Val1719Glyfs6) in 3 (including 1 with bilateral breast cancer) patients (20% of BRCA1 mutations) . BRCA2 mutations included c.1813dup(p.Ile605Asnfs 11) and c.5572del(p.Thr1858Glnfs*5) . Family history of cancer was reported in 73.9% of mutation carriers compared to 62.2% overall. Variants of uncertain significance were detected in 25.6% of patients. Two of those with the c.4484G>T BRCA1 mutation had an associated VUS in the PALB2 gene (c.365A>G(p.Asp122Gly)) . They were both under 30 and had at least 4 first- and second-degree relatives with breast and ovarian cancer. Two other patients had the same VUS in APC (c.3760A>G(p.Ile1254Val) ), all with at least 2 relatives with cancer and 1 had the BRCA1 c.4484G>T mutation and the other had no pathologic mutation identified. Conclusions: This pioneering study reveals striking cancer health disparities, with BRCA1/BRCA2 mutation frequencies exceeding rates in well-studied populations. The predominance of specific mutations and VUSs suggests population-specific genetic architecture requiring tailored approaches. Our work provides a foundation for developing culturally-appropriate cancer prevention strategies, reducing genetic testing disparities, and advancing precision medicine accessibility in vulnerable populations, ultimately contributing to the global effort to eliminate cancer health disparities.
利益披露 Disclosure
K. Chi Ndi, None.. B. Esson Mapoko, None.. V. Mouaye, None.. C. Vanvolkenburgh, None.. B. Dzekem, None.. P. Ndom, None.. D. Huo, None.. O. I. Olopade, None.

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