Age- and ethnic-driven molecular and clinical disparity of East Asian breast cancers
- Author(s)
- Ji Yoon Lee; Ji Won Lee; Min Sung Chung; Jong Gwon Choi; Sung Hoon Sim; Hyo Jeong Kim; Jeong Eun Kim; Kyoung Eun Lee; Yeon Hee Park; Myoung Joo Kang; Mi Sun Ahn; Yee Soo Chae; Ji Hyun Park; Jee Hyun Kim; Gun Min Kim; Jae Ho Byun; Keon Uk Park; Ju Won Kim; Seung Pil Jung; Jung Hyun Lee; Jung Seok An; Byunghyun Jang; Dayoung Yoon; Jiwon Kim; Jisoo Hong; Harim Koo; Kyu Ran Cho; Cheol Yong Kim; Jason K Sa; Kyong Hwa Park
- Keimyung Author(s)
- Park, Keon Uk
- Department
- Dept. of Internal Medicine (내과학)
- Journal Title
- BMC Med
- Issued Date
- 2024
- Volume
- 22
- Keyword
- Breast cancer; Ethnic diversity; Genomic alterations; Molecular subtypes; Precision medicine
- Abstract
- Background:
Breast cancer (BC) is a complex disease with profound genomic aberrations. However, the underlying molecular disparity influenced by age and ethnicity remains elusive.
Methods:
In this study, we aimed to investigate the molecular properties of 843 primary and metastatic BC patients enrolled in the K-MASTER program. By categorizing patients into two distinct age subgroups, we explored their unique molecular properties. Additionally, we leveraged large-scale genomic data from the TCGA and MSK-IMPACT studies to examine the ethnic-driven molecular and clinical disparities.
Results:
We observed a high prevalence of PI3KCA mutations in K-MASTER HER2 + tumors, particularly in older patients. Moreover, we identified increased mutation rates in DNA damage response molecules, including ARID1A, MSH6, and MLH1. The K-MASTER patients were mainly comprised of triple-negative breast cancer (TNBC) and HER2-positive tumors, while the TCGA and MSK-IMPACT cohorts exhibited a predominance of hormone receptor-positive (HR +) subtype tumors. Importantly, GATA3 mutations were less frequently observed in East Asian patients, which correlated with poor clinical outcomes. In addition to characterizing the molecular disparities, we developed a gradient-boosting multivariable model to identify a new molecular signature that could predict the therapeutic response to platinum-based chemotherapy.
Conclusions:
Our findings collectively provide unprecedented insights into the significance of age and ethnicity on the molecular and clinical characteristics of BC patients.
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