Differentiation reprogramming in gastric intestinal metaplasia and dysplasia: role of SOX 2 and CDX 2

Aims Intestinal metaplasia ( IM ), which results from de‐novo expression of CDX 2, and dysplasia are precursor lesions of gastric cancer that are associated with an increased risk for cancer development. There is much evidence suggesting a role for the transcription factor SOX 2 in gastric differentiation. The aim of this study was to attempt to establish the relationship of SOX 2 with CDX 2 and with the differentiation reprogramming that characterizes gastric carcinogenesis, to assess their involvement in IM and dysplasia. Methods and results Characterization of gastric ( SOX 2, MUC 5 AC , and MUC 6) and intestinal ( CDX 2 and MUC 2) markers in normal gastric mucosa, in 55 foci of IM and in 26 foci of dysplasia, was performed by immunohistochemistry. SOX 2 was expressed in the normal gastric mucosa, in the presumptive stem cell compartment, and was maintained in 7% of the complete ( MUC 5 AC ‐negative) and 85% of the incomplete ( MUC 5 AC ‐positive) IM subtypes. Twelve per cent of the dysplastic lesions expressed SOX 2, and the association with MUC 5 AC was lost. CDX 2 was present in all IM s and dysplastic lesions. Conclusions SOX 2 is associated with gastric differentiation in incomplete IM and is lost in the progression to dysplasia, whereas CDX 2 is acquired de novo in IM and maintained in dysplasia. This suggests that the balance between gastric and intestinal differentiation programmes impacts on the gastric carcinogenesis cascade progression.