Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
9216650 | Oral Oncology | 2005 | 19 Pages |
Abstract
Betel quid (BQ) chewing is popular in Taiwan, India, and many southeast-Asian countries. BQ chewing has strong association with the risk of oral leukoplakia (OL), oral submucous fibrosis (OSF), and oral cancer (OC). BQ components exhibit genotoxicity and may alter the structure of DNA, proteins and lipids, resulting in production of antigenicity. BQ ingredients are also shown to induce keratinocyte inflammation by stimulating the production of prostaglandins, TNF-α, IL-6, IL-8, and granulocyte-macrophage colony-stimulating factor (GM-CSF) in keratinocytes. These events may provoke tissue inflammation, early cell-mediated immunity (CMI), and immune surveillance in BQ chewers. However, BQ components also directly affect the functional activities of immunocompotent cells, and moreover tumor cells may hypo-respond to the CMI via diverse mechanisms such as induction of apoptosis of lymphocytes, induction of production of suppressor T cells, downregulation of MHC molecules in tumor cells, etc. Clinically, an alteration in lymphocyte subsets, a decrease in total number of lymphocytes, and a reduction in functional activities of CMI have been observed in isolated peripheral blood mononuclear cells (PBMC) and tumor infiltrated lymphocytes (TIL) in patients with OSF, OL or OC. Adaptation of tumor cells to immune system may promote clonal selection of resistant tumor cells, leading to immune tolerance. Future studies on effects of BQ components on CMI and humoral immunity in vitro and in vivo can be helpful for chemoprevention of BQ-related oral mucosal diseases. To elucidate how virus infection, tobacco, alcohol and BQ consumption, and other environmental exposure affect the immune status of patients with oral premalignant lesions or OC will help us to understand the immunopathogenesis of OC and to develop immunotherapeutic strategies for OC.
Keywords
AN, areca nutBQ, betel quidPAH, polyaromatic hydrocarbonsCMI, cell-mediated immunityCTL, cytotoxic T lymphocytesDC, dendritic cellHNSCC, head and neck squamous cell carcinomaLAK, lymphokine-activated killerLC, Langerhans cellLN, lymph nodeNK, natural killerPBL, peripheral blood lymphocytesROS, Reactive Oxygen SpeciesCell-mediated immunityBetel quid chewingOral cancerHead and neck cancerPBMC, peripheral blood mononuclear cellsDC, dendritic cellsOral submucous fibrosisMHC, major histocompatibility complexGSH, glutathione
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Authors
M.C. Chang, C.P. Chiang, C.L. Lin, J.J. Lee, L.J. Hahn, J.H. Jeng,