A New Insight for the Identification of Oncogenic Variants in Breast and Prostate Cancers in Diverse Human Populations, With a Focus on Latinos

Nelson M. Varela; Patricia Guevara-Ramírez; Cristian Acevedo; Tomás Zambrano; Isaac Armendáriz-Castillo; Santiago Guerrero; Luis A. Quiñones; Andrés López-Cortés

doi:10.3389/fphar.2021.630658

A New Insight for the Identification of Oncogenic Variants in Breast and Prostate Cancers in Diverse Human Populations, With a Focus on Latinos

Journal

Frontiers in Pharmacology

ISSN

1663-9812

Date Issued

2021-04-12

Author(s)

Nelson M. Varela

Patricia Guevara-Ramírez

Cristian Acevedo

Tomás Zambrano

Isaac Armendáriz-Castillo

Facultad de Ciencias de la Salud Eugenio Espejo

Santiago Guerrero

Facultad de Ciencias de la Salud Eugenio Espejo

Luis A. Quiñones

Andrés López-Cortés

Facultad de Ciencias de la Salud Eugenio Espejo

DOI

10.3389/fphar.2021.630658

Abstract

Background: Breast cancer (BRCA) and prostate cancer (PRCA) are the most commonly diagnosed cancer types in Latin American women and men, respectively. Although in recent years large-scale efforts from international consortia have focused on improving precision oncology, a better understanding of genomic features of BRCA and PRCA in developing regions and racial/ethnic minority populations is still required.Methods: To fill in this gap, we performed integrated in silico analyses to elucidate oncogenic variants from BRCA and PRCA driver genes; to calculate their deleteriousness scores and allele frequencies from seven human populations worldwide, including Latinos; and to propose the most effective therapeutic strategies based on precision oncology.Results: We analyzed 339,100 variants belonging to 99 BRCA and 82 PRCA driver genes and identified 18,512 and 15,648 known/predicted oncogenic variants, respectively. Regarding known oncogenic variants, we prioritized the most frequent and deleterious variants of BRCA (n = 230) and PRCA (n = 167) from Latino, African, Ashkenazi Jewish, East Asian, South Asian, European Finnish, and European non-Finnish populations, to incorporate them into pharmacogenomics testing. Lastly, we identified which oncogenic variants may shape the response to anti-cancer therapies, detailing the current status of pharmacogenomics guidelines and clinical trials involved in BRCA and PRCA cancer driver proteins.Conclusion: It is imperative to unify efforts where developing countries might invest in obtaining databases of genomic profiles of their populations, and developed countries might incorporate racial/ethnic minority populations in future clinical trials and cancer researches with the overall objective of fomenting pharmacogenomics in clinical practice and public health policies.

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A New Insight for the Identification of Oncogenic Variants in Breast and Prostate Cancers in Diverse Human Populations, With a Focus on Latinos