Alpha-enolase (ENO1) is an evolutionally-conserved protein and a key glycolytic enzyme. ENO1 is found on the tumor cell surfaces and functions as one of the plasminogen receptors. Then it further degrades fibrin and several extracellular matrix components. It is implicating that it may be involved in tissue invasion during tumor metastasis. In recent years, upregulation of ENO1 gene has been observed in several highly tumorigenic or metastatic cell lines, including small cell lung cancer, head and neck cancer. In addition, its overexpression has been also suggested to be a prognostic biomarker in several types of human cancers such as non-small cell lung cancer, pancreatic carcinoma, hepatitis C virus -related hepatocellular carcinoma and breast cancer. In veterinary medicine, recently published research revealed that overexpression of ENO1 is detected in tumor cells of canine mammary carcinoma and significantly correlated with shorter survival. Based on previous study, we follow the canine mammary carcinoma study to investigate the ENO1 expression in other tumors and to verify whether ENO1 expression statuses are related to their malignancy or poor outcome. In this study, we investigated the ENO1 expression by immunohistochemistry and quantified by Quick score. Correlations of ENO1 overexpression and clinicopathologic parameters of tumors were examined by Pearson's chi-square test. Cause-specific survival was calculated by Kaplan-Meier analysis to verify whether ENO1 expression statuses can be a prognostic factor of other tumors. Four common tumors in dogs and cats including squamous cell carcinoma (SCC), mast cell tumor (MCT), lymphoma, and melanoma were retrospectively retrieved with their clinical and pathological information. A total of 38 cases of SCCs (31 dogs and 7 cats), 59 cases of MCTs (54 dogs and 5 cats), 32 cases of lymphomas (25 dogs and 7 cats) and 57 cases of canine melanomas were included. The results revealed that in canine SCCs, ENO1 overexpression was significantly correlation with higher grade, poorer tumor cell differentiation and shorter cause-specific survival. In canine lymphomas, ENO1 overexpression was significantly correlation with shorter cause-specific survival. In canine MCTs, ENO1 overexpression was significantly correlation with younger age. In canine melanomas, ENO1 overexpression was significantly correlation with poorer cell differentiation, higher mitotic activity and shorter cause-specific. Thus, ENO1 overexpression may be used as a biomarker for poorer prognosis in canine SCCs, lymphomas and melanomas.