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BDDN: bayesian dynamic differential network analysis in cancer proteomics

Authors
 Kim, Juan  ;  Lee, Doyeon  ;  Park, Jina  ;  Jin, Ick Hoon  ;  Ha, Min Jin 
Citation
 BMC BIOINFORMATICS, Vol.27(1), 2026-02 
Article Number
 78 
Journal Title
BMC BIOINFORMATICS
ISSN
 1471-2105 
Issue Date
2026-02
Keywords
Cancer proteomics ; Protein-protein interaction ; Dynamic differential network ; Bayesian precision regression model
Abstract
Motivation Cancer progression and treatment responses are governed by intricate
and dynamic molecular interactions. Although differential network analysis offers considerable potential for identifying condition-specific changes in protein-protein interactions, existing methods primarily rely on static comparisons between groups and do not adequately model underlying biological dynamics. This limitation restricts the ability to detect gradual and complex molecular responses to therapeutic interventions.
Results We propose a Bayesian dynamic differential network model to infer time-resolved changes in protein-protein interactions. Applied to cancer proteomics data, our approach captures gradual shifts in differential protein-protein interactions between experimental groups that standard group-based approaches fail to detect The inferred differential networks reveal protein pairs with time-varying interaction patterns between groups, highlighting critical changes associated with drug response. Subsequent analyses, including functional clustering and hub identification, uncover distinct trajectories among differential edges and pinpoint key proteins that mediate pivotal transitions in the dynamic structure of the differential networks.
Conclusions The proposed Bayesian dynamic differential network model successfully characterizes temporal variations in protein-protein interactions following drug intervention. The method uncovers time-dependent interaction patterns that differ between experimental groups, providing enhanced insights into drug-induced molecular mechanisms. This framework facilitates the identification of critical regulatory proteins and demonstrates broad applicability across diverse time-course omics investigations.
Files in This Item:
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DOI
10.1186/s12859-026-06371-w
Appears in Collections:
5. Graduate School of Transdisciplinary Health Sciences (융합보건의료대학원) > Graduate School of Transdisciplinary Health Sciences (융합보건의료대학원) > 1. Journal Papers
Yonsei Authors
Ha, Min Jin(하민진)
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/211816
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