Hoffmann et al. investigated the association of diet with fungal populations, using fecal samples from 98 healthy individuals [158]. They characterized 62 fungal genera and 184 species by deep sequencing, and usually found that the presence of either the phyla Ascomycota or Basiodiomycota was mutually exclusive. The authors could not conclude which of those fungi are true gut residents selleck compound and which are passengers resulting from diet. We cannot exclude the possibility that the presence of Saccharomyces is due to the ingestion of yeast-containing foods such as bread and beer [82].
A recent study conducted on the Wayampi Amerindian community showed a high diversity among yeast species in the gut, with a prevalence of S. cerevisiae over Candida species [80], suggesting a role for
this fungus in gut immune homeostasis. Thus, integrating information on the repertoire of the gut mycobiota in the context of the broader microbiota and developing functional tests to measure its role in shaping immune function is necessary to better understand the role of the microbial communities in sustaining human health. Although we have described BIBW2992 research buy the composition of the fungal microbiota in various locations in the human body, we remain aware that these locations are not isolated and that DCs trained in the Peyer’s patches of the intestine (Fig. 1) can shape T-cell responses in other locations. A clear example of this crosstalk was recently shown in an elegant study by Kim et al. [159], who showed that antibiotic treatment of mice increases susceptibility to allergic airway disease by promoting varying degrees of fungal outgrowth in the intestine, ultimately resulting in the acquisition of an M2 phenotype by alveolar macrophages [159]. The authors isolated C. parapsilosis
from the feces of antibiotic-treated mice and showed that transferring this fungus to mice that did not carry this species increased their susceptibility to allergic airway inflammation induced by papain or house dust mite extract [159]. Oral treatment of mice with Candida species isolated from humans also led to fungal outgrowth in the gut and exacerbated allergic airway inflammation, increasing serum levels Mirabegron of prostaglandin E2, which promoted the development of M2 macrophages [159]. The mycobiota alteration mediated imbalance in alveolar macrophage function contributed to the increase in airway inflammation, as untreated animals receiving alveolar macrophages from antibiotic-treated mice developed more severe airway inflammation than animals that received alveolar macrophages from control mice. Based on this result, it appears that intestinal dysbiosis, particularly the altered ratio of fungi to bacteria, could be a causative factor in the development of allergic disease. Patients with severe asthma with fungal sensitization are often sensitized to C. albicans and benefit from antifungal drug therapy [160]. Colonization of mice with C.