4.7 Article

Somatic and Germline Genomic Alterations in Very Young Women with Breast Cancer

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CLINICAL CANCER RESEARCH
卷 28, 期 11, 页码 2339-2348

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AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1078-0432.CCR-21-2572

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  1. Susan G. Komen
  2. Breast Cancer Research Foundation
  3. Susan Smith Executive Council

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The study identified significant differences in somatic alterations of three genes (PIK3CA, GATA3, and ARID1A) in young versus older women with luminal A breast cancer. Additionally, a portion of young women with breast cancer carried pathogenic germline variants, with BRCA1/2 mutations being the most common. Further investigation into these genetic differences may help improve treatment options for young patients with breast cancer.
Purpose: Young age at breast cancer diagnosis correlates with unfavorable clinicopathologic features and worse outcomes compared with older women. Understanding biological differences between breast tumors in young versus older women may lead to better therapeutic approaches for younger patients. Experimental Design: We identified 100 patients <= 35 years old at nonmetastatic breast cancer diagnosis who participated in the prospective Young Women's Breast Cancer Study cohort. Tumors were assigned a surrogate intrinsic subtype based on receptor status and grade. Whole-exome sequencing of tumor and germline samples was performed. Genomic alterations were compared with older women (>= 45 years old) in The Cancer Genome Atlas, according to intrinsic subtype. Results: Ninety-three tumors from 92 patients were successfully sequenced. Median age was 32.5 years; 52.7% of tumors were hormone receptor-positive/HER2-negative, 28.0% HER2-positive, and 16.1% triple-negative. Comparison of young to older women (median age 61 years) with luminal A tumors (N = 28 young women) revealed three significant differences: PIK3CA alterations were more common in older patients, whereas GATA3 and ARID1A alterations were more common in young patients. No significant genomic differences were found comparing age groups in other intrinsic subtypes. Twenty-two patients (23.9%) in the Young Women's Study cohort carried a pathogenic germline variant, most commonly (13 patients, 14.1%) in BRCA1/2. Conclusions: Somatic alterations in three genes (PIK3CA, GATA3, and ARID1A) occur at different frequencies in young versus older women with luminal A breast cancer. Additional investigation of these genes and associated pathways could delineate biological susceptibilities and improve treatment options for young patients with breast cancer.

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