Background/Aim: DJ-1, an oncogenic molecule, helps to maintain somatic stem cells by reducing the intracellular level of reactive oxygen species (ROS). This study investigated the role of DJ-1 in glioma stem cells (GSCs). Materials and Methods: U87-MG (U87) and U251-MG (U251) glioblastoma cell lines that express wild-type and mutant p53, respectively, were used. These were cultured with DJ-1-targeting siRNA and subjected to a variety of in vitro experiments or intracranial transplantation into nude mice. Results: Knockdown of DJ-1 reduced clonogenicity only in U87 cells, which was rescued by p53 depletion. ROS accumulated in DJ-1-depleted cells, although treatment with N-acetyl cysteine, which quenches ROS, did not affect exhaustion of CSCs among U87 cells by DJ-1 knockdown. In a serial transplantation study, DJ-1 knockdown prolonged the survival of mice in secondary transplantation. Conclusion: DJ-1 plays a pivotal role in maintenance of stem cell self-renewal in the U87 cell line. Glioblastoma (GBM), defined as a grade IV astrocytoma, is the most aggressive and commonly diagnosed brain cancer and accounts for 16% of all primary brain and central nervous system neoplasms (1, 2). The current standard treatment protocol for GBM is surgery, followed by temozolomide chemotherapy and radiotherapy. A variety of novel drugs have been developed; however, the median survival of patients with GBM who receive any therapy is only 15 months (3).Among several factors responsible for these poor outcomes, traditional therapies are ineffective against cancer stem cells (CSCs). CSCs are postulated to be a small population of cells located at the top of the cellular hierarchy that supply other tumor cells by undergoing self-renewal and differentiation (CSC hypothesis) (4, 5). Glioma stem cells (GSCs) were first identified as CD133-expressing cells with high tumorigenicity in vivo and resistance to current therapy (6). This implies that GSCs can initiate cancer recurrence and metastasis. Consequently, molecular strategies targeting GSCs must be urgently developed to treat GBM.Parkinsonism-associated deglycase (PARK7, DJ-1) functions in anti-apoptotic signaling and protein quality control in response to oxidative stress. Failure of these functions due to genetic mutations is associated with the early-onset and familial form of Parkinson's disease (7). DJ-1 was originally cloned as an oncogene that enhances RAS-driven neoplastic transformation (8). Moreover, DJ-1 is overexpressed in many types of cancer and this contributes to survival, proliferation, and metastasis of cancer cells (9-11). However, the functional role of DJ-1 in maintenance of GSCs remains elusive.CSCs and somatic stem cells share many characteristics that are established by common molecular mechanisms (12). The Mortalin/DJ-1 complex sustains the stemness of hematopoietic stem cells, one of the most characterized types of somatic stem cells, by modulating mitochondrial oxidative stress (13). We hypothesized that this mechanism also operates in GSCs. The present study...