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Inferring Gene-Phenotype Associations via Global Protein Complex Network Propagation

Author

Listed:
  • Peng Yang
  • Xiaoli Li
  • Min Wu
  • Chee-Keong Kwoh
  • See-Kiong Ng

Abstract

Background: Phenotypically similar diseases have been found to be caused by functionally related genes, suggesting a modular organization of the genetic landscape of human diseases that mirrors the modularity observed in biological interaction networks. Protein complexes, as molecular machines that integrate multiple gene products to perform biological functions, express the underlying modular organization of protein-protein interaction networks. As such, protein complexes can be useful for interrogating the networks of phenome and interactome to elucidate gene-phenotype associations of diseases. Methodology/Principal Findings: We proposed a technique called RWPCN (Random Walker on Protein Complex Network) for predicting and prioritizing disease genes. The basis of RWPCN is a protein complex network constructed using existing human protein complexes and protein interaction network. To prioritize candidate disease genes for the query disease phenotypes, we compute the associations between the protein complexes and the query phenotypes in their respective protein complex and phenotype networks. We tested RWPCN on predicting gene-phenotype associations using leave-one-out cross-validation; our method was observed to outperform existing approaches. We also applied RWPCN to predict novel disease genes for two representative diseases, namely, Breast Cancer and Diabetes. Conclusions/Significance: Guilt-by-association prediction and prioritization of disease genes can be enhanced by fully exploiting the underlying modular organizations of both the disease phenome and the protein interactome. Our RWPCN uses a novel protein complex network as a basis for interrogating the human phenome-interactome network. As the protein complex network can capture the underlying modularity in the biological interaction networks better than simple protein interaction networks, RWPCN was found to be able to detect and prioritize disease genes better than traditional approaches that used only protein-phenotype associations.

Suggested Citation

  • Peng Yang & Xiaoli Li & Min Wu & Chee-Keong Kwoh & See-Kiong Ng, 2011. "Inferring Gene-Phenotype Associations via Global Protein Complex Network Propagation," PLOS ONE, Public Library of Science, vol. 6(7), pages 1-11, July.
    • Handle: RePEc:plo:pone00:0021502
    DOI: 10.1371/journal.pone.0021502
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    Cited by:

    1. Yadong Dong & Yongqi Sun & Chao Qin, 2018. "Predicting protein complexes using a supervised learning method combined with local structural information," PLOS ONE, Public Library of Science, vol. 13(3), pages 1-23, March.
    2. Peng Yang & Xiaoli Li & Hon-Nian Chua & Chee-Keong Kwoh & See-Kiong Ng, 2014. "Ensemble Positive Unlabeled Learning for Disease Gene Identification," PLOS ONE, Public Library of Science, vol. 9(5), pages 1-11, May.
    3. MaoQiang Xie & YingJie Xu & YaoGong Zhang & TaeHyun Hwang & Rui Kuang, 2015. "Network-based Phenome-Genome Association Prediction by Bi-Random Walk," PLOS ONE, Public Library of Science, vol. 10(5), pages 1-18, May.

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