Our first experiments consisted of treating samples of dental plaque with cortisol at a concentration found in the saliva of patients with periodontitis.14,16 As a control for these experiments we used dental plaque that was incubated under the same conditions as the treatment samples but without cortisol added to the saliva used as the medium. People with periodontal disease present higher levels of cortisol in the gingival crevicular fluid,14 a serum exudate in direct contact with the oral microbiome. After only 2 h of incubation in the presence of cortisol, we proceed to perform the analysis, avoiding possible changes related to the growth of individual members of the microbiome and not to the presence of the hormone itself (see Methods section in the Supplementary Information accompanying this manuscript). We assigned the phylogenetic origin of those sequences using Kraken,17 and phylogenetic profiles were used to identify significant differences between active communities under the different conditions studied by performing linear discriminant analysis (LDA) effect size (LEfSe). In our study, LEfSe determines the active members of the oral microbiome, based on changes in the number of transcripts, that most likely explain differences between the two biological conditions tested (presence and absence of cortisol). LEfSe robustly identifies features that are statistically different among biological classes using the non-parametric factorial Kruskal-Wallis (KW) sum-rank test and subsequently uses a set of pairwise tests among subclasses using the (unpaired) Wilcoxon rank-sum test for biological consistency. Finally, LDA estimates the effect size of each differentially abundant taxonomic group.18 Among all the organisms in the oral community, members of the phylum Fusobacteria (class Fusobacteriia and order Fusobacteriales) were significantly more active (increased the number of transcripts significantly) after the addition of cortisol (Fig. 1). Among them, one species, Leptotrichia goodfellowii, was substantially more active (Fig. 1b). Species belonging to the Fusobacteriales, such as Fusobacterium nucleatum have been associated with a wide variety of human diseases, other than periodontitis, including adverse pregnancy outcome, GI disorders (e.g., colorectal cancer, inflammatory bowel disease), cardiovascular disease, rheumatoid arthritis, and respiratory tract infections.19 Leptotrichia species are typically part of the commensal flora in the oral cavity and genitourinary tract and are seldom found in clinically significant specimens. However, Leptotrichia has been found to be in higher proportion in gingivitis.20,21

Fig. 1 Distinct active taxa identified using LEfSe analysis. Metatranscriptome hit counts were obtained using Kraken against an oral microbiome database. Counts were then analyzed using LEfSe to identify significant differences at the species level between the microbial communities compared. a Cladogram constructed using the LEfSe method to indicate the phylogenetic distribution of active bacteria that were remarkably enriched. Red represented the enriched taxa the untreated microbial community and green represented the enriched taxa in the microbial community treated with cortisol. b LDA (Linear Discriminant Analysis) scores showed significant bacterial differences within groups at different taxonomic levels. Red represented the enriched taxa in the untreated microbial community and green represented the enriched taxa in the microbial community treated with cortisol Full size image

Next, we looked at how cortisol influenced the profiles of expression of the oral microbiome. To this end, we performed enrichment of Gene Ontology (GO) terms analysis, and we observed that, after only 2 h of exposure to the hormone, the profiles of activities of the whole community had already changed and they were similar to the profiles of expression we previously found in periodontitis progression.22,23 Among them GO terms associated with proteolysis, oligopeptide transport, iron metabolism, and flagellum assembly were over-represented in the presence of cortisol (Fig. 2a). What is more important these activities have been associated with an increase in pocket depth, and essential clinical parameter in periodontitis, during the progression of the disease.23 Interestingly, GO terms linked to response to host immune response were also over-represented when cortisol was present, even though the microbiome in our samples was not in contact with host cells (Fig. 2a). As previously indicated potassium ion transport was significantly under-represented when cortisol was added (Fig. 2b), mimicking our in vivo observations of periodontitis progression.23 In a follow-up manuscript, we demonstrated that ion potassium is a signal in functional dysbiosis of periodontal disease.24

Fig. 2 Changes in functional profiles in the oral microbiome treated with cortisol. We used Gene Ontology (GO) enrichment analysis to assess the oral microbiome functional response to the presence of added cortisol to the medium. Enriched terms obtained using GOseq were summarized and visualized as a scatter plot using REVIGO. Only GO terms with FDR adjusted p-value < 0.05 in the ‘GOseq’ analysis were used. a Over-represented functional activities in the presence of cortisol summarized as GO terms related to biological processes. b Over-represented functional activities in the absence of cortisol summarized as GO terms related to biological processes. Circle size is proportional to the frequency of the GO terms; color indicates the log10 p-value (red higher, blue lower). The distance between circles represents GO terms’ semantic similarities. Each of the circles represents a GO term, which depending on the similarity in the terms included in them they will be closer or more distant in the graph. In red are activities we have previously seen associated with periodontitis and its progression.22,23 Full size image

Interestingly, when we look at the activities associated explicitly with putative virulence factors, we found a similar pattern of over-represented GO terms related to the addition of cortisol (Sup. Figure 1). Although phylum Fusobacteria was the phylogenetic group that increased its transcriptional activity more significantly, the rest of the microbiome showed a shift in its profile of expression. Thus, the more significant fraction of up-regulated putative virulence factors seems to be synthesized by members of the genus Streptococcus (Sup. Figure 2). We observed similar results in our two previous studies on periodontitis progression23 and the effect of ion potassium in functional dysbiosis of the oral microbiome.24 As a whole, these results seem to indicate that the presence of cortisol leads to a community-wide response very similar to the one observed in vivo during periodontitis.

We then used a simpler system based on our previous results on the community-wide transcriptome results. To this end, we performed transcriptome analysis of the effect of cortisol on pure culture of organisms that we identified as more active in the presence of cortisol (Fig. 1): Leptotrichia goodfellowii and Fusobacterium nucleatum, which is a representative of the order Fusobacteriales and an essential member of the oral microbiome. In just 2 h of exposure, there was a shift in their transcriptome profiles. F. nucleatum showed an increase in biological processes GO terms associated with proteolysis, cobalamin biosynthesis and iron transport (Sup. Fig. 3a), which we have previously found associated with the progression of periodontal disease.22,23 In the case of L. goodfellowii, we also found activities related to iron ion transport (Sup. Fig. 3b). The intersection of metabolic events that were commonly altered in F. nucleatum and L. goodfellowii was associated with the growth of the organisms such as lipid A biosynthesis, DNA replication or translation (Sup. Fig 3), which indicates activation of their metabolism.

Moreover, iron transport was also altered in both organisms in the presence of cortisol (Sup. Fig 3). These results are in agreement with the effects observed for the whole oral microbiome where members of the Fusobacteriales order are more active when cortisol was added to the medium, (Fig. 1). Likewise, the intersection of common molecular functions enriched with the addition of cortisol in F. nucleatum and L. goodfellowii include iron acquisition (iron-ion binding and iron-ion transmembrane transporter activity) and peptidase activities (serine-type endopeptidase activity) (Sup. Fig. 4).

Altogether, these results show that the only exposure to cortisol in the oral microbiome is enough to cause a significant shift in the gene expression profile of the community mimicking community-wide expression profiles observed in periodontitis and its progression in vivo.22,23 Our results also highlight the importance of Fusobacteria and Leptotrichia as the members of the community that more rapidly increase their metabolism in response to an increase of cortisol in the environment.

Though it has been known for a long time that hormones had some effect on the metabolism of bacteria,7,25,26,27 the mechanisms by which this cross-talk happens to remain mostly unknown. As we deepen our understanding of the precise roles of the microbiome in health and disease, we expect that new mechanisms will be shown to involve host hormones, including novel interactions. The present manuscript builds on the idea that human hormones can be used by the microbiome as signals to sense changes in their environment thus modifying its expression profile to fit the new conditions better. Nonetheless, we should recognize that given the limited number of samples in this pilot study, further work with a larger sample size should be performed to confirm the results presented in this manuscript.

Using a metatranscriptomic analysis would allow us to assess the direct effect that hormones have on the metabolism of the microbial community. Approaching the host-microbiome interactions from a microbial endocrinology-based point may provide an understanding of the specific pathways by which microorganisms may influence the outcome of certain infections and chronic diseases.