Expression and Significance of MyD88 in Patients With Gastric Cardia Cancer in a High-Incidence Area of China

Background:Gastric cardia cancer (GCC) arises in the area of the stomach adjoining the esophageal-gastric junction and has unique risk factors. It was suggested that the involvement ofHelicobacter pyloriis associated with GCC from high-risk population. Myeloid differentiation factor 88 (MyD88) is a crucial adaptor molecule in Toll-like signaling pathway recognizingH. pylori. Its role in GCC has not been elucidated yet. In this study, our purpose is to investigate the expression and significance of MyD88 in GCC tissue. Methods:Expression of MyD88 and nuclear factor kappa B (NF-kappa B) p105/p50 and infection ofH. pyloriwere detected by immunohistochemistry in gastric cardia tissue. The correlation of MyD88 expression to NF-kappa B p105/p50 expression,H. pyloriinfection, and clinicopathologic characteristics in gastric cardia tissue was analyzed. The involvement of MyD88 in patient prognosis was also analyzed. Results:Our data showed that the expression of MyD88 elevated from normal mucosa to inflammation (p= 0.071). The expression of MyD88 was enhanced in GCC tissues by contrast to non-malignant cardia mucosa (p= 0.025). What's more, overexpression of MyD88 was detected in intestinal-type adenocarcinoma with inflammation. Patients with high MyD88 staining revealed a better differentiation (p= 0.02). MyD88 also positively correlated with NF-kappa B p105/p50 expression (p= 0.012) in cancer tissue. Expression of MyD88 was increased but not significantly in biopsies withH. pyloriinfection compared with non-infected biopsies. Multivariate analyses revealed lymph node metastasis but not MyD88 expression was an independent predictor for patient survival. Conclusion:These findings provide pathological evidence that upregulating MyD88 and inducing inflammation might be involved in gastric cardia carcinogenesis in high-risk population. MyD88 plays a role in gastric cardia carcinogenesis with NF-kappa B pathway activation. Higher MyD88 expression is not a major prognostic determinant in GCC, but it may relate to the tumor cell differentiation.