This work was supported by grants from The State Key Laboratory of Proteomics(SKLP-O200811), The National Natural Science Foundation of China (60603054, 30800200, 30621063), National Basic Research Program of China (2006CB910803, 2006CB910706, 2010CB912700), Hi-Tech Research and Development Program of China (2006AA02A312) and National S&T Major Project (2008ZX10002-016, 2009ZX09301- 002)
The huge datasets produced from high-throughput microarray technology can elucidate unknown mechanisms of gene regulation in biological systems. Because biological processes are dynamic, it is relevant to focus on certain condition-specific gene regulatory sub-networks. The cell cycle is a basic cellular process, thus, identifying cell cycle specific regulatory sub-networks in yeast will provide a basis for understanding the cell cycle and may be important in other cellular conditions. With a gene expression differential equation model (GEDEM), dynamic cell cycle-related regulatory relationships were indentified from a static regulatory network. Compared to cell cycle-related regulatory interactions previously published, this method identified more true regulatory relationships and show higher performance than other methods. On larger datasets, the GEDEM identified regulatory sub-networks with high sensitivity and specificity. Further analysis on combinatorial regulation revealed that condition-specific regulatory sub-networks exhibited more significant correlations between transcription factors than previously implied in static network analyses, which infer that the condition-specific sub-networks are closer to reality than static network. Additionally, the GEDEM identified more potential co-regulatory transcriptional factors in the cell cycle.
LIU Qi-Jun, WANG Zheng-Hua, LIU Wan-Lin, LI Dong, HE Fu-Chu, ZHU Yun-Ping. A Novel Method to Identify The Condition-specific Regulatory Sub-network That Controls The Yeast Cell Cycle Based on Gene Expression Model[J]. Progress in Biochemistry and Biophysics,2010,37(4):402-415
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