Neuroblastoma was a solid tumor originated from undifferentiated neural crest cells. However, some neuroblastoma can regress without any remedy, indicating the pathological complexity of this tumor. Notch is a surface receptor that plays a key role in the tumorgenesis of neuroblastoma. We have previousely demonstrated that inhibition of Notch signaling causes neuronal differentiation of neuroblastoma, and induces the expression of a favorable prognostic marker, calreticulin (CRT). We thus proposed to address the molecular mechanism underlying the Notch-dependent regulation of CRT expression in neuroblastoma cells. To determine whether transcription of CRT is subject to the regulation by Notch signaling, by using real-time PCR, we demonstrated that the CRT mRNA levels were significantly enhanced by the inhibition of Notch in a neuroblastoma cell line SH-SY5Y. Moreover, we identified a putative binding motif of HERP, a Notch responsive gene, within the CRT promoter region. Consistent with this finding, a luciferase reporter gene construct encoding this CRT promoter sequence was shown to be responsive to the inhibition of Notch signaling. To further test whether CRT indeed plays an important role in the differentiation of neuroblastoma cells, we employed a RNAi approach to down-regulate CRT expression in SH-SY5Y cells and found that the down-regulation of CRT significantly hindered the neuronal differentiation of neuroblastoma cells induced by a Notch signal inhibitor and retinoic acid. Our findings strongly suggest that CRT critically involves in a mechanism governing the Notch signaling mediated differentiation of neuroblastoma through transcriptional regulation of CRT gene expression.