BackgroundKidney renal clear cell carcinoma (KIRC) is a prevalent type of urological malignancy. The present study aimed to predict biomarkers for KIRC.MethodsWe collected transcriptomic and clinical information for KIRC from The Cancer Genome Atlas and GSE22541 cohorts.ResultsUnsupervised clustering of 35 epithelial–mesenchymal transformation (EMT)‐related differentially expressed gene profiles divided samples into two clusters with distinct immune characteristics. Six genes (IL20RB, DDC, ANKRD36BP2, F2RL1, TEK, and AMN) were found to construct a prognostic risk model using multivariate Cox regression analysis. Kaplan–Meier analysis suggested the better prognosis of the KIRC patients in the low‐risk group than that in the high‐risk group. Immune infiltration analyses was conducted using xCell and single‐sample gene set enrichment analysis, indicating that the risk score was associated with the immune microenvironment of the KIRC. Prognostic marker gene‐targeted medications with high drug sensitivity were predicted in KIRC patients.ConclusionsIn summary, the present study identified IL20RB, DDC, ANKRD36BP2, F2RL1, TEK, and AMN as prognostic biomarkers, providing insight into immunotherapy and gene‐targeted drugs of KIRC.