Our data revealed that adding AFP resulted in inhibition of IL-12

Our data revealed that adding AFP resulted in inhibition of IL-12 production at the transcriptional level, not by decreased expression of TLRs. Although the regulation of transcription of IL-12p40 and IL-12p35

has been elucidated in various studies [23,24], the detailed mechanism of inhibition of IL-12 transcription by AFP remains unclear. Further study is needed to clarify the detailed mechanism of inhibition Tanespimycin cost of IL-12 by AFP. Taken together, IL-12 might play a mainly essential role in the impairment of NK activity by AFP. To evaluate the possibility of involvement of other immunosuppressive cytokines inhibiting NK activity, we examined the IL-6 and IL-10 levels in the supernatants of the co-cultures of NK cells and AFP-DCs/Alb-DCs by specific ELISAs. IL-6 levels in the supernatants of AFP-DCs were similar to those of Alb-DCs, and IL-10 levels in the supernatants of

AFP-DCs were significantly lower than those of Alb-DCs (M. Yamamoto, unpublished data). These results suggest that the addition of AFP might impair the ability Buparlisib of cytokine production of DCs. In a previous report, Um et al. demonstrated that AFP impairs the function of dendritic cells and induces their apoptosis [13]. In their report, they used the commercially available human cord blood AFP. Thus, we used human cord blood AFP because this is the only commercially available AFP. The carbohydrates of AFP are heterogeneous, which is reflected by differences in the binding of individual Gemcitabine nmr AFP molecules to lectins. Therefore, we also added the supernatants of Huh7 cells, AFP-producing HCC cells or control medium on the DCs and evaluated IL-12 production after LPS stimulation by specific ELISA. The supernatants of Huh7 cells contained AFP (1·76 µg/ml) and control medium contained no AFP. The IL-12 production of DCs co-cultured with the supernatants of Huh7 cells was significantly lower than that with control medium (M. Yamamoto, unpublished data). These results were consistent with the results using human cord blood AFP.

Although we cannot deny the possibility that unknown factors, except AFP, in the supernatants of Huh7 cell might affect the IL-12 production of DCs, these results suggest that another type of AFP might also have immunoregulatory ability on DCs. In this study, we demonstrate that AFP might down-regulate IL-12 production from DCs which inhibit NK activity. Zhang et al. demonstrated that IL-12 improves the cytotoxicity of NK cells via up-regulated expression of NKG2D on NK cells [25]. We have demonstrated previously that NKG2D expression on NK cells was down-regulated in the progression of chronic liver disease, including HCC [18], which suggested that NK activities were impaired in HCC patients. The expression of NKG2D on NK cells in HCC patients with high serum AFP was significantly lower than those in HCC patients with low serum AFP (M. Yamamoto, unpublished data).

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