Supplemental Table S4 from Evaluation of Multiple Breast Cancer Polygenic Risk Score Panels in Women of Latin American Heritage

Descripción del Articulo

A substantial portion of the genetic predisposition for breast cancer is explained by multiple common genetic variants of relatively small effect. A subset of these variants, which have been identified mostly in individuals of European (EUR) and Asian ancestries, have been combined to construct a po...

Descripción completa

Detalles Bibliográficos
Autores: Huang, Xiaosong, Lott, Paul C., Hu, Donglei, Zavala, Valentina A., Jamal, Zoeb N., Vidaurre, Tatiana, Casavilca Zambrano, Sandro Angel Aníbal, Navarro Vásquez, Jeannie, Castañeda, Carlos A., Valencia, Guillermo, Morante, Zaida, Calderón, Mónica, Abugattas, Julio E., Fuentes, Hugo A., Liendo-Picoaga, Ruddy, Cotrina, Jose M., Neciosup, Silvia P., Rioja Viera, Patricia, Salinas, Luis A., Galvez-Nino, Marco, Huntsman, Scott, Sanchez, Sixto E., Williams, Michelle A., Gelaye, Bizu, Estrada-Florez, Ana P., Polanco-Echeverry, Guadalupe, Echeverry, Magdalena, Velez, Alejandro, Carmona-Valencia, Jenny A., Bohorquez-Lozano, Mabel E., Torres, Javier, Cruz, Miguel, Ho, Weang-Kee, Hwang Teo, Soo, Chee Tai, Mei, John, Esther M., Haiman, Christopher A., Conti, David V., Chen, Fei, Torres-Mejía, Gabriela, Kushi, Lawrence H., Neuhausen, Susan L., Ziv, Elad, Carvajal-Carmona, Luis G., Fejerman, Laura
Fecha de Publicación:2025
Institución:Universidad Nacional Mayor de San Marcos
Repositorio:UNMSM-Tesis
Lenguaje:inglés
OAI Identifier:oai:cybertesis.unmsm.edu.pe:20.500.12672/27548
Enlace del recurso:https://hdl.handle.net/20.500.12672/27548
https://doi.org/10.1158/1055-9965.28358092
Nivel de acceso:acceso abierto
Materia:Cáncer
Cáncer - Prevención
Epidemiología
https://purl.org/pe-repo/ocde/ford#3.01.04
https://purl.org/pe-repo/ocde/ford#3.02.21
https://purl.org/pe-repo/ocde/ford#5.01.02
Descripción
Sumario:A substantial portion of the genetic predisposition for breast cancer is explained by multiple common genetic variants of relatively small effect. A subset of these variants, which have been identified mostly in individuals of European (EUR) and Asian ancestries, have been combined to construct a polygenic risk score (PRS) to predict breast cancer risk, but the prediction accuracy of existing PRSs in Hispanic/Latinx individuals (H/L) remain relatively low. We assessed the performance of several existing PRS panels with and without addition of H/L-specific variants among self-reported H/L women. PRS performance was evaluated using multivariable logistic regression and the area under the ROC curve. Both EUR and Asian PRSs performed worse in H/L samples compared with original reports. The best EUR PRS performed better than the best Asian PRS in pooled H/L samples. EUR PRSs had decreased performance with increasing Indigenous American (IA) ancestry, while Asian PRSs had increased performance with increasing IA ancestry. The addition of two H/L SNPs increased performance for all PRSs, most notably in the samples with high IA ancestry, and did not impact the performance of PRSs in individuals with lower IA ancestry. A single PRS that incorporates risk variants relevant to the multiple ancestral components of individuals from Latin America, instead of a set of ancestry-specific panels, could be used in clinical practice. The results highlight the importance of population-specific discovery and suggest a straightforward approach to integrate ancestry-specific variants into PRSs for clinical application.
Supplemental Table S4 from Evaluation of Multiple Breast Cancer Polygenic Risk Score Panels in Women of Latin American Heritage
Nota importante:
La información contenida en este registro es de entera responsabilidad de la institución que gestiona el repositorio institucional donde esta contenido este documento o set de datos. El CONCYTEC no se hace responsable por los contenidos (publicaciones y/o datos) accesibles a través del Repositorio Nacional Digital de Ciencia, Tecnología e Innovación de Acceso Abierto (ALICIA).

Ejemplares Similares