Abstract
To clarify the significance of p73 in Epstein‐Barr virus (EBV)‐associated gastric carcinoma (GC), the immunohistochemical expression and CpG‐island methylation of p73 were evaluated in cancer tissues and adjacent nonneoplastic tissues of GC with and without EBV infection. Loss of p73 expression by immunohistochemistry was specific to EBV‐associated GC (11/13) compared to EBV‐negative GC (3/38), which was independent of abnormal p53 expression. With methylation‐specific polymerase chain reaction (MSP), the aberrant methylation of p73 exon 1 was similarly specific to EBV‐associated GC (12/13), and also rare in EBV‐negative GC (2/38). Bisulfite sequencing for p73 exon 1 and its 5′ region confirmed the MSP results, showing uniform and high‐density methylation in EBV‐associated GC. Comparative MSP analysis of p14, p16 and p73 methylation, using 20 cases each of formalin‐fixed and paraffin‐embedded tissues of early GC with and without EBV infection, confirmed 2 types of methylation: global methylation with increased rates (p14 and p16) and specific methylation of p73 in EBV‐associated GC. In nonneoplastic mucosa, p14, p16 and p73 methylation occurred in both EBV‐associated (8/33, 6/34 and 3/38, respectively) and EBV‐negative GC (6/23, 4/35, and 1/35). p73 methylation was observed in the mucosa without H. pylori infection in all 4 samples. Loss of p73 expression through aberrant methylation of the p73 promoter occurs specifically in EBV‐associated GC, together with the global methylation of p14 and p16. A specific type of gastritis, prone to a higher grade of atrophy and p73 methylation, may facilitate the development of EBV‐associated GC. © 2006 Wiley‐Liss, Inc.