| Literature DB >> 34743578 |
Min-Hua Rong1, Jian-Di Li1, Lu-Yang Zhong1, Yu-Zhen Huang1, Juan Chen1, Li-Yuan Xie1, Rong-Xing Qin1, Xiao-Lian He1, Zhan-Hui Zhu1, Su-Ning Huang2, Xian-Guo Zhou1.
Abstract
In our studies, cyclin B1 (CCNB1) mRNA and protein were overexpressed in hepatocellular carcinoma (HCC) tissues compared with non-HCC tissues. Moreover, CCNB1 was overexpressed in the serum of HCC patients. The expression of CCNB1 was associated with several crucial clinicopathologic characteristics, and the HCC patients with overexpressed CCNB1 had worse overall survival outcomes. In the screening of interactional genes, a total of 266 upregulated co-expression genes, which were positively associated with CCNB1, were selected from the datasets, and 67 downregulated co-expression genes, which were negatively associated with CCNB1, were identified. The key genes might be functionally enriched in DNA replication and the cell cycle pathways. CDC20, CCNA2, PLK1, and FTCD were selected for further research because they were highly connected in the protein-protein interaction networks. Upregulated CDC20, CCNA2, and PLK1 and downregulated FTCD might result in undesirable overall survival outcomes for HCC patients. The univariate Cox analysis results showed that CDC20 and PLK1 might be two independent risk factors, while FTCD might be protective in HCC. Therefore, CCNB1 may participate in the cell cycle of HCC by regulating DNA replication, and CCNB1 may provide a direction for the diagnosis of early-stage HCC and targeted HCC therapy.Entities:
Keywords: Cyclin B1; DNA replication; cell cycle; hepatocellular carcinoma; prognosis; weighted gene co-expression network analysis
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Year: 2021 PMID: 34743578 PMCID: PMC8919315 DOI: 10.1177/15353702211049149
Source DB: PubMed Journal: Exp Biol Med (Maywood) ISSN: 1535-3699