期刊
IEEE ACCESS
卷 8, 期 -, 页码 9578-9586出版社
IEEE-INST ELECTRICAL ELECTRONICS ENGINEERS INC
DOI: 10.1109/ACCESS.2019.2963537
关键词
Protein interaction network; essential protein; topology; protein complex
资金
- National Natural Science Foundation of China [11361033]
- Natural Science Foundation of Gansu Province [1212RJZA029]
The recognition of essential proteins not only can help to understand the mechanism of cell operation, but also help to study the mechanism of biological evolution. At present, many scholars have been discovering essential proteins according to the topological structure of protein network and complexes. While some proteins still can not be recognized. In this paper, we proposed two new methods complex degree centrality (CDC) and complex in-degree and betweenness definition (CIBD) which integrate the local character of protein complexes and topological properties to determine the essentiality of proteins. First, we give the definitions of complex average centrality (CAC) and complex hybrid centrality (CHC) which both describe the properties of protein complexes. Then we propose these new methods CDC and CIBD based on CAC and CHC definitions. In order to access these two methods, different Protein-Protein Interaction (PPI) networks of Saccharomyces cerevisiae, DIP, MIPS and YMBD are used as experimental materials. By comparing with the competing methods including DC, BC, LAC, SC, EC, SoECC and the recent method LBCC and IBC, our experimental results in networks show that the methods of CDC and CIBD can help to improve the precision of predicting essential proteins.
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