Differential whole-genome doubling based signatures for improvement on clinical outcomes and drug response in patients with breast cancer

Yingli Lv; Guotao Feng; Lei Yang; Xiaoliang Wu; Chengyi Wang; Aokun Ye; Shuyuan Wang; Chaohan Xu; Hongbo Shi

doi:10.1016/j.heliyon.2024.e28586

Differential whole-genome doubling based signatures for improvement on clinical outcomes and drug response in patients with breast cancer

Heliyon. 2024 Mar 26;10(7):e28586. doi: 10.1016/j.heliyon.2024.e28586. eCollection 2024 Apr 15.

Authors

Yingli Lv¹, Guotao Feng¹, Lei Yang¹, Xiaoliang Wu¹, Chengyi Wang¹, Aokun Ye¹, Shuyuan Wang¹, Chaohan Xu¹, Hongbo Shi¹

Affiliation

¹ College of Bioinformatics Science and Technology, Harbin Medical University, Harbin, Heilongjiang, 150081, China.

Abstract

Whole genome doublings (WGD), a hallmark of human cancer, is pervasive in breast cancer patients. However, the molecular mechanism of the complete impact of WGD on survival and treatment response in breast cancer remains unclear. To address this, we performed a comprehensive and systematic analysis of WGD, aiming to identify distinct genetic alterations linked to WGD and highlight its improvement on clinical outcomes and treatment response for breast cancer. A linear regression model along with weighted gene co-expression network analysis (WGCNA) was applied on The Cancer Genome Atlas (TCGA) dataset to identify critical genes related to WGD. Further Cox regression models with random selection were used to optimize the most useful prognostic markers in the TCGA dataset. The clinical implication of the risk model was further assessed through prognostic impact evaluation, tumor stratification, functional analysis, genomic feature difference analysis, drug response analysis, and multiple independent datasets for validation. Our findings revealed a high aneuploidy burden, chromosomal instability (CIN), copy number variation (CNV), and mutation burden in breast tumors exhibiting WGD events. Moreover, 247 key genes associated with WGD were identified from the distinct genomic patterns in the TCGA dataset. A risk model consisting of 22 genes was optimized from the key genes. High-risk breast cancer patients were more prone to WGD and exhibited greater genomic diversity compared to low-risk patients. Some oncogenic signaling pathways were enriched in the high-risk group, while primary immune deficiency pathways were enriched in the low-risk group. We also identified a risk gene, ANLN (anillin), which displayed a strong positive correlation with two crucial WGD genes, KIF18A and CCNE2. Tumors with high expression of ANLN were more prone to WGD events and displayed worse clinical survival outcomes. Furthermore, the expression levels of these risk genes were significantly associated with the sensitivities of BRCA cell lines to multiple drugs, providing valuable insights for targeted therapies. These findings will be helpful for further improvement on clinical outcomes and contribution to drug development in breast cancer.

Keywords: Drug response; Prognosis genes; WGD-Related genes; Whole-genome doubling.