ADH1B型
免疫系统
生物
小桶
药物代谢
癌症研究
基因
氟达拉滨
药品
基因表达
免疫学
环磷酰胺
药理学
遗传学
转录组
酶
化疗
生物化学
支链α-酮酸脱氢酶复合物
脱氢酶
作者
Zhijie Xu,Bi Peng,Fanhua Kang,Wen-Qin Zhang,Muzhang Xiao,Jianbo Li,Qianhui Hong,Yuan Cai,Wei Liu,Yuanliang Yan,Jinwu Peng
标识
DOI:10.3389/fcell.2022.877254
摘要
Background: The different pharmacological effects of drugs in different people can be explained by the polymorphisms of drug metabolism-related genes. Emerging studies have realized the importance of drug metabolism-related genes in the treatment and prognosis of cancers, including ovarian cancer (OV). In this study, using comprehensive bioinformatics and western blot, we identified that the drug metabolism-related gene, ADH1B, was significantly down-regulated in OV cells and tissues. The patients with a high level of ADH1B presented a good prognosis. We also found a negative correlation between ADH1B expression and the activity of chemotherapeutic agents, such as cyclophosphamide. In addition, positive correlations were observed between ADH1B expression and multiple immune checkpoints, including LAG3 and HAVCR2. The immune infiltration analysis further indicated that aberrantly expressed ADH1B might have important roles in regulating the infiltration of macrophages and neutrophils in OV tissues. Then, the co-expression analysis was conducted and the top three enriched KEGG pathways were spliceosome, RNA transport, and DNA replication. In conclusion, the drug metabolism-related gene ADH1B and its interactive network play an essential role in the immune regulation and therapeutic response and maybe identified as promising therapeutic targets for OV patients.
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