Construction and analysis of protein-protein interaction networks based on proteomics data of prostate cancer

Chen,Chen; Shen,Hong; Zhang,Li-Guo; Liu,Jian; Cao,Xiao-Ge; Yao,An-Liang; Kang,Shao-San; Gao,Wei-Xing; Han,Hui; Cao,Feng-Hong; Li,Zhi-Guo

doi:10.3892/ijmm.2016.2577

Construction and analysis of protein-protein interaction networks based on proteomics data of prostate cancer

Authors:
- Chen Chen
- Hong Shen
- Li-Guo Zhang
- Jian Liu
- Xiao-Ge Cao
- An-Liang Yao
- Shao-San Kang
- Wei-Xing Gao
- Hui Han
- Feng-Hong Cao
- Zhi-Guo Li
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Affiliations: Department of Urology, North China University of Science and Technology Affiliated Hospital, Tangshan, Hebei 063000, P.R. China, Department of Modern Technology and Education Center, North China University of Science and Technology and International Science and Technology Cooperation Base of Geriatric Medicine, Tangshan, Hebei 063000, P.R. China, Tianjin Binhai New Area Hangu No. 1 High School, Tianjin 300480, P.R. China, Medical Research Center, North China University of Science and Technology and International Science and Technology Cooperation Base of Geriatric Medicine, Tangshan, Hebei 063000, P.R. China
Published online on: April 26, 2016 https://doi.org/10.3892/ijmm.2016.2577
Pages: 1576-1586
Copyright: © Chen et al. This is an open access article distributed under the terms of Creative Commons Attribution License.

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Abstract

Currently, using human prostate cancer (PCa) tissue samples to conduct proteomics research has generated a large amount of data; however, only a very small amount has been thoroughly investigated. In this study, we manually carried out the mining of the full text of proteomics literature that involved comparisons between PCa and normal or benign tissue and identified 41 differentially expressed proteins verified or reported more than 2 times from different research studies. We regarded these proteins as seed proteins to construct a protein-protein interaction (PPI) network. The extended network included one giant network, which consisted of 1,264 nodes connected via 1,744 edges, and 3 small separate components. The backbone network was then constructed, which was derived from key nodes and the subnetwork consisting of the shortest path between seed proteins. Topological analyses of these networks were conducted to identify proteins essential for the genesis of PCa. Solute carrier family 2 (facilitated glucose transporter), member 4 (SLC2A4) had the highest closeness centrality located in the center of each network, and the highest betweenness centrality and largest degree in the backbone network. Tubulin, beta 2C (TUBB2C) had the largest degree in the giant network and subnetwork. In addition, using module analysis of the whole PPI network, we obtained a densely connected region. Functional annotation indicated that the Ras protein signal transduction biological process, mitogen-activated protein kinase (MAPK), neurotrophin and the gonadotropin-releasing hormone (GnRH) signaling pathway may play an important role in the genesis and development of PCa. Further investigation of the SLC2A4, TUBB2C proteins, and these biological processes and pathways may therefore provide a potential target for the diagnosis and treatment of PCa.

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