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The presence of high level soluble herpes virus entry mediator in sera of gastric cancer patients
Authors:Heo Sook-Kyoung  Ju Seong-A  Kim Gyu Yeol  Park Sang-Min  Back Sung Hun  Park Neung-Hwa  Min Young Joo  An Won G  Nguyen Thi Thu-Ha  Kim Sun-Min  Kim Byung-Sam
Affiliation:Department of Biological Sciences University of Ulsan Ulsan 680-749, Korea.
Abstract:The development of gastric cancer (GC) is closely related to chronic inflammation caused by Helicobacter pylori infection, and herpes virus entry mediator (HVEM) is a receptor expressed on the surface of leukocytes that mediates potent inflammatory responses in animal models. However, the role of HVEM in human GC has not been studied. Previously, we showed that the interaction of HVEM on human leukocytes with its ligand LIGHT induces intracellular calcium mobilization, which results in inflammatory responses including induction of proinflammatory cytokine production and anti-bacterial activities. In this study, we report that leukocytes from GC patients express lower levels of membrane HVEM (mHVEM) and have lower LIGHT-induced bactericidal activities than those from healthy controls (HC). In contrast, levels of soluble HVEM (sHVEM) in the sera of GC patients were significantly higher than in those of HC. We found that monocyte membrane-bound HVEM is released into the medium when cells are activated by proinflammatory cytokines such as TNF-α and IL-8, which are elevated in the sera of GC patients. mHVEM level dropped in parallel with the release of sHVEM, and release was completely blocked by the metalloprotease inhibitor, GM6001. We also found that the low level of mHVEM on GC patient leukocytes was correlated with low LIGHT-induced bactericidal activities against H. pylori and S. aureus and production of reactive oxygen species. Our results indicate that mHVEM on leukocytes and sHVEM in sera may contribute to the development and/or progression of GC.
Keywords:cytokines   inflammation   monocytes   receptors   tumor necrosis factor   member 14   stomach neoplasms   TNFSF14 protein   human
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