Abstract Background: The palate is the most common site for intraoral minor salivary gland tumors. This study was aimed to present the clinicopathological features of a series of 133 benign and malignant palatal minor salivary gland tumors. Methods: In this study, 133 benign and malignant palatal minor salivary gland tumors were retrieved from the files of Department of Pathology, National Taiwan University Hospital from January, 1993 to December, 2009. The clinicopathological features and their correlations of these 133 palatal minor salivary gland tumors were analyzed and reported. Results: There were 78 (58.6%) benign and 55 (41.4%) malignant minor salivary gland tumors in the palate. Pleomorphic adenoma (PA, 74 cases), mucoepidermoid carcinoma (MEC, 26 cases), and adenoid cystic carcinoma (ACC, 18 cases) constituted 89% of all tumors. PA patients showed a marked female predominance (2:1) and a mean age of 47 years. Histopathologically, there were 47 classic and 27 cellular PAs. Of the 74 PAs, 12 were completely-encapsulated, 40 partially-encapsulated, and 22 non-encapsulated. Plasmacytoid myoepithelial cell, clear cell, squamous epithelial nest, keratin pearl, hyalinized stroma, osteoid area, and chondroid area were found in 50, 19, 29, 19, 49, 8, and 6 PAs, respectively. MEC patients also demonstrated a significant female predilection (2.7:1) and a mean age of 43 years. The majority of MEC patients had T1 or T2 (69%) and stage 1 or stage 2 tumors (69%) at the initial presentation. Of the 26 MEC patients, only one had regional lymph node metastasis, one distant metastasis, and one recurrence of the tumor after treatment. Moreover, only one MEC patient died 1 year after treatment. Thus, the 2-year, 5-year and 10-year survival rates were all 96% for MEC patients. Histologically, 13 MECs were classified as low-grade, 4 intermediate-grade, and 9 high-grade tumors. Perineural invasion was noted in 2 MECs. High-grade MECs occurred commonly in older patients (> 50 years old) and low-grade MECs frequently affected younger patients (≦ 50 years old, P = 0.046). The ACC patients, however, revealed a slight male predominance (1:0.8) and a mean age of 54 years. Two-thirds of ACC patients showed T4 and stage 4 tumors. Moreover, 7 ACC patients had distant metastases, but only 2 had regional lymph node metastases. Local recurrence was noted in 6 ACCs after treatment. The 2-year, 5-year and 10-year survival rates were 100%, 72% and 56% for ACC patients, respectively. Of the 18 ACCs, 11 were classified as cribriform type, 3 tubular type, and 4 solid type. Perineural invasion was present in 13 ACCs. Statistical analyses showed that patients with tubular or solid ACCs were more likely to have T3 or T4 tumors (P = 0.057), stage 3 or stage 4 disease (P = 0.057), local recurrence of the tumor (P = 0.023), and poorer overall survival (P = 0.013). ACCs with perineural invasion were prone to present as T3 or T4 (P = 0.022) and stage 3 or stage 4 tumors (P = 0.022). Moreover, T3 or T4 (P = 0.038) and stage 3 or stage 4 (P = 0.038) ACCs more frequently showed distant metastases. Larger ACCs (T3 and T4, P = 0.054) and advanced stage ACCs (stage 3 and stage 4, P = 0.054) were prone to have local recurrence after treatment. In addition, older ACC patients (> 50 years, P = 0.025) were more frequent to have poorer overall survival. Conclusion: We conclude that PA is the most common benign and MEC and ACC are the two most frequent malignant palatal minor salivary gland tumors. Both PA and MEC patients have a prominent female predilection, but ACC patients have a slight male preponderance. The mean age of ACC patients is much older than that of PA or MEC patients. The prognosis of palatal MEC patients is better than that of palatal ACC patients. Two-thirds of ACC patients show T4 and stage 4 tumors at the initial presentation. ACCs are prone to have distant metastases rather than regional lymph node metastasis. Perineural invasion is frequently present in ACCs. In addition, patients with tubular or solid ACCs are more likely to have larger tumors, advanced stages, local recurrence, and poorer overall survival.