Ranking candidate genes of esophageal squamous cell carcinomas based on differentially expressed genes and the topological properties of the co-expression network.

[esophageal squamous cell carcinoma]

The aim of this study was to identify the candidate genes of esophageal squamous cell carcinoma (ESCC ).Gene expression profiling of 17 ESCC samples and 17 adjacent normal samples , GSE 20347 , was downloaded from Gene Expression Omnibus database . The raw data were preprocessed , and the differentially expressed genes (DEGs ) between ESCC and normal samples were identified by using SAM software (false discovery rate <0 .001 ). Then , the co -expression network of DEGs was constructed based on Pearson 's correlation test (r-value ≥0 .8 ). Furthermore , the topological properties of the co -expression network were analyzed through NetworkAnalyzer (default settings ) of Cytoscape . The expression fold changes of DEGs and topological properties were utilized to identify the candidate genes of ESCC (Crin score >4 ), which were further analyzed based on DAVID functional enrichment analysis (P-value <0 .05 ).A total of 1 ,063 DEGs were identified , including 490 up-regulated and 573 down-regulated DEGs . Then , the co -expression network of DEGs was constructed , containing 999 nodes and 46 ,323 edges . Based on the expression fold changes of DEGs and the topological properties of the co -expression network , DEGs were ranked , and the top 24 genes were candidate genes of ESCC , such as CRISP 3 , EREG , CXCR 2 , and CRNN . Furthermore , the 24 genes were significantly enriched in bio-functions regarding cell differentiation , glucan biosynthetic process and immune response .The present study suggested that CRISP 3 , EREG , CXCR 2 , and CRNN might be causative genes of ESCC , and play vital roles in the development of ESCC . However , further experimental studies are needed to confirm our results .