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KMID : 0381120110330020197
Genes and Genomics
2011 Volume.33 No. 2 p.197 ~ p.204
Biased over-expression of CD4? natural killer T cells induces the expansion of marginal zone B cells in aged V¥á14 TCR transgenic C57BL/6 mice
Lee Sung-Won

Youm Bo-Hyun
Kim Sun-Mi
Seo Han-Hyung
Park Hyun-Jung
Hong Seok-Mann
Abstract
Marginal zone B (MZB) cells play an important role in the host defense against blood-borne pathogens. Recently, it has been reported that MZB cells amplify dendritic cell-mediated activation of natural killer T (NKT) cells, suggesting that MZB cells are required for optimal NKT cell stimulation. Prior studies have led us to test whether the increased levels of NKT cells would have an immunological impact on MZB cells. To this end, we employed V¥á14 TCR transgenic (tg) mice and found that MZB cells were 2 to 3 times more abundant in these mice, compared with wild-type mice, at 15 weeks of age. In addition, this expansion of MZB cells was not observed in young (5-week-old) V¥á14 TCR tg mice, implying that aging is one of the factors regulating MZB cell expansion. Because NKT cells consist of heterogeneous subsets with distinct immunological functions, we next examined whether there were any alterations to the frequencies of individual NKT subpopulations. Interestingly, V¥á14 TCR tg mice manifested a biased increase in levels of CD4? NKT cells. These cells are known to produce IFN¥ã, which may explain the unexpected expansion of MZB cells in V¥á14 TCR tg mice, because IFN¥ã has been reported to activate MZB cells to produce IL10. Taken together, our results demonstrate that the specific increase in numbers of CD4? NKT cells may contribute to MZB cell expansion.
KEYWORD
Natural killer T cell, Marginal zone B cell, V¥á14 TCR transgenic mice, ¥á-GalCer
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