Glioma is one of the most common primary brain tumors. Its conventional treatments such as surgical resection or radiation fail to increase the survival of patients. Induction of differentiation is one way for controlling the malignant growth of glioma. Rat C6 glioma is a rapidly proliferating cell line with oligodendrocytic, astrocytic, and neuronal properties. Based on the cancer stem cell hypothesis, in this study, we use C6 tumor sphere cells, together with parental adhesion cells, to investigate the regulation of differentiation-inducing agent, N6-O'2-dibutyryl cAMP (dbcAMP). The efficacy of treatment was examined by phase-contrast microscopy, Immunocytochemistry, Western blot, RT-PCR and Real Time Quantitative PCR. After dbcAMP treatment, morphological changes of C6 cells could be easily observed. Most of the adhesion cells showed bipolar shape, which are similar to glial progenitors. Compared with adhesion cells, sphere cells exposed to dbcAMP also extended processes, and some cells resulted in a stellar shape. The morphology more closely resembled mature astrocyte or neuron. Astrocytic marker glial fibrillary acidic protein (GFAP) expression increased in tumorsphere. Interestingly, the specific neuronal marker ßⅢ-tubulin immunopositive cells were also observed. Meanwhile, the neural stem cell marker nestin decreased relatively. Our results suggest that the formation of tumor sphere model, which has cancer stem-like cells potential, could be a suitable approach to identify the initiation and progression of rat C6 glioma cells.