Identifying cooperating cancer driver genes in individual patients through hypergraph random walk

Tong Zhang; Shao-Wu Zhang; Ming-Yu Xie; Yan Li

doi:10.1016/j.jbi.2024.104710

Identifying cooperating cancer driver genes in individual patients through hypergraph random walk

J Biomed Inform. 2024 Sep:157:104710. doi: 10.1016/j.jbi.2024.104710. Epub 2024 Aug 17.

Authors

Tong Zhang¹, Shao-Wu Zhang², Ming-Yu Xie³, Yan Li³

Affiliations

¹ Key Laboratory of Information Fusion Technology of Ministry of Education, School of Automation, Northwestern Polytechnical University, Xi'an 710072, China; School of Electrical and Mechanical Engineering, Pingdingshan University, Pingdingshan 467000, China.
² Key Laboratory of Information Fusion Technology of Ministry of Education, School of Automation, Northwestern Polytechnical University, Xi'an 710072, China. Electronic address: [email protected].
³ Key Laboratory of Information Fusion Technology of Ministry of Education, School of Automation, Northwestern Polytechnical University, Xi'an 710072, China.

PMID: 39159864
DOI: 10.1016/j.jbi.2024.104710

Abstract

Objective: Identifying cancer driver genes, especially rare or patient-specific cancer driver genes, is a primary goal in cancer therapy. Although researchers have proposed some methods to tackle this problem, these methods mostly identify cancer driver genes at single gene level, overlooking the cooperative relationship among cancer driver genes. Identifying cooperating cancer driver genes in individual patients is pivotal for understanding cancer etiology and advancing the development of personalized therapies.

Methods: Here, we propose a novel Personalized Cooperating cancer Driver Genes (PCoDG) method by using hypergraph random walk to identify the cancer driver genes that cooperatively drive individual patient cancer progression. By leveraging the powerful ability of hypergraph in representing multi-way relationships, PCoDG first employs the personalized hypergraph to depict the complex interactions among mutated genes and differentially expressed genes of an individual patient. Then, a hypergraph random walk algorithm based on hyperedge similarity is utilized to calculate the importance scores of mutated genes, integrating these scores with signaling pathway data to identify the cooperating cancer driver genes in individual patients.

Results: The experimental results on three TCGA cancer datasets (i.e., BRCA, LUAD, and COADREAD) demonstrate the effectiveness of PCoDG in identifying personalized cooperating cancer driver genes. These genes identified by PCoDG not only offer valuable insights into patient stratification correlating with clinical outcomes, but also provide an useful reference resource for tailoring personalized treatments.

Conclusion: We propose a novel method that can effectively identify cooperating cancer driver genes for individual patients, thereby deepening our understanding of the cooperative relationship among personalized cancer driver genes and advancing the development of precision oncology.

Keywords: Cooperating cancer driver genes; Hypergraph random walk; Individual patients; Personalized cancer driver genes; Personalized hypergraph.

MeSH terms

Algorithms*
Computational Biology / methods
Databases, Genetic
Gene Expression Profiling / methods
Gene Expression Regulation, Neoplastic
Gene Regulatory Networks
Humans
Mutation
Neoplasms* / genetics
Precision Medicine / methods
Signal Transduction / genetics