An epileptic seizure is a common presenting symptom of glioma, or epilepsy may develop later during the disease. Epileptic seizures affect the quality of life in patients with glioma. Good seizure control during 6-12months follow-up has been associated with gross total resection, radiation therapy and chemotherapy of gliomas. Little is known about seizure control during long-term follow-up and about factors which may affect the prognosis of epilepsy in glioma patients. We identified retrospectively all adult patients with diffuse glioma (grade 2-4) associated epilepsy (n=123) living in Helsinki, who received treatment at Helsinki University Hospital neuro-oncology center during 2013-2015. We excluded patients with histopathological diagnosis prior to 2005. Data was collected from medical records for five years after diagnosis of glioma, or until death. In this patient cohort 49 (39.8%) had grade 2 glioma, 19 (15.4%) had grade 3 glioma and 55 (44.7%) had grade 4 glioma. 29 (23.6%) of tumors were astrocytomas, 24 (19.5%) were oligoastrocytomas, 15 (12.2%) were oligodendrogliomas and 55 (44.7%) were glioblastomas. A seizure was the presenting symptom in 87 (70.7%) of the patients. The majority, 68 (57.6%) patients were seizure-free for at least 12months at some point during follow-up and 47 (39.8%) patients were seizure-free during the last year of follow-up. Survival for five years from glioma diagnosis (p<0.001), lower grade of tumor (p<0.001), IDH mutation (p<0.001), epilepsy as first symptom (p<0.001), younger age (p<0.001) and lack of progression (p = 0.021) correlated with seizure freedom at the end of follow-up. When the results were analyzed separately in survivors and deceased patients, only progression correlated negatively with seizure freedom at the end of follow-up in surviving patients (p = 0.008). In 5-year survivors, longer seizure-free periods were achieved by patients without progression of glioma (p = 0.040) vs patients with progression, or without focal aware (p 0.003) or focal impaired awareness seizures (p = 0.002) vs patients with only focal to bilateral tonic-clonic seizures. In deceased patients, progression (p<0.001) and lower grade of glioma (p = 0.003) correlated positively and focal aware seizures negatively (p = 0.021) with a longer seizure-free period. In all patients, freedom of seizures at the end of follow-up was less likely for patients who had focal aware (p = 0.015) than for patients without focal aware seizures. There are differences in seizure-free times in patients with grade 2-4 glioma and epilepsy. The results suggest that the prognosis of glioma may be the most important factor influencing the prognosis of epilepsy.