Very recently, Saijo et al. reported that dectin-2 is a crucial receptor for the α-mannan from C. albicans and plays an important role in host defense against this fungus. Cytokine production and signal transduction by α-mannan from C. albicans are completely abolished in dectin-2−/− mice compared to wild-type mice (28). This implies that the pathogenic effect of CMWS could be exhibited via dectin-2. However, this possibility needs further examination. The present study strongly suggests that C. metapsilosis, a less pathogenic fungus than C. albicans, can cause coronary arteritis, such as that observed during KD, and fungal-induced
learn more sepsis in the same way as C. albicans. Since CMWS only contains α-mannosyl residue (not expressed as β-mannan), the results of this study support our previous results. However, further studies are needed because the precise mechanism(s) behind these pathogenic activities is not understood. Nevertheless, these findings suggest the possibility of a novel strategy for drug therapy; that is, regulation
of the biosynthesis of Candida mannan Selleckchem Bortezomib could be a candidate for therapy of coronary arteritis and acute anaphylactoid shock. We thank Miki Arai for technical assistance. This work was supported by the Program for Promotion of Basic and Applied Researches for Innovations in Bio-oriented Industry (BRAIN). “
“Animals lacking the inducible nitric oxide synthase gene (nos2−/−) acetylcholine are less susceptible to Mycobacterium avium strain 25291 and lack nitric oxide-mediated immunomodulation of CD4+ T cells. Here we show that the absence of nos2 results in increased accumulation of neutrophils and both CD4+ and CD8+ T cells within the M. avium containing granuloma. Examination of the T-cell phenotype in M. avium infected mice demonstrated that CD4+CD44hi effector T cells expressing the Th1 transcriptional regulator T-bet (T-bet+) were specifically reduced by the presence of nitric oxide. Importantly, the T-bet+ effector population could be separated into
CD69hi and CD69lo populations, with the CD69lo population only able to accumulate during chronic infection within infected nos2−/− mice. Transcriptomic comparison between CD4+CD44hiCD69hi and CD4+CD44hiCD69lo populations revealed that CD4+CD44hiCD69lo cells had higher expression of the integrin itgb1/itga4 (VLA-4, CD49d/CD29). Inhibition of Nos2 activity allowed increased accumulation of the CD4+CD44hiT-bet+CD69lo population in WT mice as well as increased expression of VLA-4. These data support the hypothesis that effector T cells in mycobacterial granulomata are not a uniform effector population but exist in distinct subsets with differential susceptibility to the regulatory effects of nitric oxide.