QIGTD: identifying critical genes in the evolution of lung adenocarcinoma with tensor decomposition

Bolin Chen; Jinlei Zhang; Ci Shao; Jun Bian; Ruiming Kang; Xuequn Shang

doi:10.1186/s13040-024-00386-w

BioData Mining (Sep 2024)

QIGTD: identifying critical genes in the evolution of lung adenocarcinoma with tensor decomposition

Bolin Chen,
Jinlei Zhang,
Ci Shao,
Jun Bian,
Ruiming Kang,
Xuequn Shang

Affiliations

Bolin Chen: School of Computer Science, Northwestern Polytechnical University
Jinlei Zhang: School of Computer Science, Northwestern Polytechnical University
Ci Shao: School of Computer Science, Northwestern Polytechnical University
Jun Bian: Department of General Surgery, Xi’an Children’s Hosptial, Xi’an Jiaotong University Affiliated Children’s Hosptial
Ruiming Kang: Rewise (Hangzhou) Information Technology Co., LTD
Xuequn Shang: School of Computer Science, Northwestern Polytechnical University

DOI: https://doi.org/10.1186/s13040-024-00386-w
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 14

Abstract

Read online

Abstract Background Identifying critical genes is important for understanding the pathogenesis of complex diseases. Traditional studies typically comparing the change of biomecules between normal and disease samples or detecting important vertices from a single static biomolecular network, which often overlook the dynamic changes that occur between different disease stages. However, investigating temporal changes in biomolecular networks and identifying critical genes is critical for understanding the occurrence and development of diseases. Methods A novel method called Quantifying Importance of Genes with Tensor Decomposition (QIGTD) was proposed in this study. It first constructs a time series network by integrating both the intra and inter temporal network information, which preserving connections between networks at adjacent stages according to the local similarities. A tensor is employed to describe the connections of this time series network, and a 3-order tensor decomposition method was proposed to capture both the topological information of each network snapshot and the time series characteristics of the whole network. QIGTD is also a learning-free and efficient method that can be applied to datasets with a small number of samples. Results The effectiveness of QIGTD was evaluated using lung adenocarcinoma (LUAD) datasets and three state-of-the-art methods: T-degree, T-closeness, and T-betweenness were employed as benchmark methods. Numerical experimental results demonstrate that QIGTD outperforms these methods in terms of the indices of both precision and mAP. Notably, out of the top 50 genes, 29 have been verified to be highly related to LUAD according to the DisGeNET Database, and 36 are significantly enriched in LUAD related Gene Ontology (GO) terms, including nuclear division, mitotic nuclear division, chromosome segregation, organelle fission, and mitotic sister chromatid segregation. Conclusion In conclusion, QIGTD effectively captures the temporal changes in gene networks and identifies critical genes. It provides a valuable tool for studying temporal dynamics in biological networks and can aid in understanding the underlying mechanisms of diseases such as LUAD.

Published in BioData Mining

ISSN: 1756-0381 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General): Computer applications to medicine. Medical informatics; Science: Mathematics: Analysis
Website: https://biodatamining.biomedcentral.com/

About the journal

Abstract

Keywords