作者:
Han ShuwenYang XiZhou QingZhuang JingWu WeiHuzhou Univ
Huzhou Cent Hosp Affiliated Cent Hosp Dept Oncol Huzhou Peoples R China Huzhou Univ
Huzhou Cent Hosp Affiliated Cent Hosp Dept Nursing Huzhou Peoples R China Huzhou Univ
Grad Sch Nursing Huzhou Peoples R China Huzhou Univ
Huzhou Cent Hosp Affiliated Cent Hosp Dept Gastroenterol 198 Hongqi Rd Huzhou 313000 Zhejiang Peoples R China
Background Early diagnosis of liver metastasis is of great importance for enhancing the survival of colorectal adenocarcinoma (CAD) patients, and the combined use of a single biomarker in a classier model has shown gr...
详细信息
Background Early diagnosis of liver metastasis is of great importance for enhancing the survival of colorectal adenocarcinoma (CAD) patients, and the combined use of a single biomarker in a classier model has shown great improvement in predicting the metastasis of several types of cancers. However, it is little reported for CAD. This study therefore aimed to screen an optimal classier model of CAD with liver metastasis and explore the metastatic mechanisms of genes when applying this classier model. Methods The differentially expressed genes between primary CAD samples and CAD with metastasis samples were screened from the Moffitt Cancer Center (MCC) dataset . The classification performances of six selected algorithms, namely, LR, RF, SVM, GBDT, NN, and catboost, for classification of CAD with liver metastasis samples were compared using the MCC dataset by detecting their classification test accuracy. In addition, the consortium datasets of and were used as internal and external validation sets to screen the optimal method. Subsequently, functional analyses and a drug-targeted network construction of the feature genes when applying the optimal method were conducted. Results The optimal catboost model with the highest accuracy of 99%, and an area under the curve of 1, was screened, which consisted of 33 feature genes. A functional analysis showed that the feature genes were closely associated with a "steroid metabolic process" and "lipoprotein particle receptor binding" (eg APOB and APOC3). In addition, the feature genes were significantly enriched in the "complement and coagulation cascade" pathways (eg FGA, F2, and F9). In a drug-target interaction network, F2 and F9 were predicted as targets of menadione. Conclusion The catboost model constructed using 33 feature genes showed the optimal classification performance for identifying CAD with liver metastasis.
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