Nasopharyngeal Carcinoma (NPC) is one of the most common cancers among Chinese living in southern China, Hong Kong, Singapore and Taiwan. The cause of the disease is quite complex, and the molecular mechanisms involved in the pathogenesis of NPC still are not yet well defined. Although it was proposed that Epstein-Barr virus (EBV) is closely associated with NPC pathogenesis, but recently many studies have reported that EBV behaves more likely as progression factors but not initiation factors. The purpose of this research was to find out the genes associated with NPC pathogenesis. Using cDNA microarray analysis of mRNA expression between NPC cell lines and normal nasal mucosal epithelial cells, SOX5 gene expression was found significantly increased in NPC cell lines by quantitative RT-PCR and Western blot analysis. In our previous studies of the function of SOX-5 gene in NPC, we found that Ribosomal Protein L37 (RpL37) was also significantly increased in NPC cell lines, especially in NPC-TW01N1 and NPC-TW06N1 cell lines. To further identify the relationship between SOX5 and RpL37, we performed some investigation to clarify this condition. We found that SOX5 and RpL37 gene expressions could be reciprocally regulated in NPC cells and suggested that RpL37 may be a critical factor for the growth of NPC tumors. To study the role of RpL37 in the molecular pathogenesis of NPC and its functions, we used a stable shRpL37 lentivirus infected NPC-TW01N1 cell lines. We found that the expression of RpL37 mRNA and protein was downregulated remarkably in these call lines. This gene could promote tumor cell migration, proliferation and invasion in vitro. In addition, the down-regulation of RpL37 could up-regulate the expression of p53. We know that p53 is a suppressor gene which could affect the cell cycle. We used flow cytometry to analyze the difference between cell lines with or without shRpL37 infected. Finally, we found that the S-phase cells treated by shRpL37 lentivirus decreased about 28% than NPC-TW01N1 cell lines without infection. However, in NOD/SCID mice bearing shRpL37 infected NPC xenograft, the tumor growth and metastatic activity were moderately increased, and the weights of shRpL37 infected NOD/SCID mice were obviously decreased at last week. We also found those NOD/SCID mice were not healthy when sacrified, their intestinal tract showed focal ulceration and almost no stool in the large intestine. It is concluded that the downregulation of RpL37 gene may play a role to promote the formation of nasopharyngeal carcinoma of nasopharynx and as a suppressor gene in NPC pathogenesis to affect NPC migration, proliferation and invasion in addition to it chemotactic property.