Modulatory Influence of Segmented Filamentous Bacteria on Transcriptomic Response of Gnotobiotic Mice Exposed to TCDD

• Published in: Frontiers in microbiology Vol. 8; p. 1708
• Main Authors: Stedtfeld, Robert D., Chai, Benli, Crawford, Robert B., Stedtfeld, Tiffany M., Williams, Maggie R., Xiangwen, Shao, Kuwahara, Tomomi, Cole, James R., Kaminski, Norbert E., Tiedje, James M., Hashsham, Syed A.
• Format: Journal Article
• Language: English
• Published: Switzerland Frontiers Media S.A 07.09.2017
• Subjects: gnotobiotic mice; gut dysbiosis; host microbe response; Microbiology; regulatory T-cells; segmented filamentous bacteria; TCDD; segmented filamentous bacteria; B. fragilis; TCDD; gnotobiotic mice; host microbe response; regulatory T-cells; gut dysbiosis
• ISSN: 1664-302X; 1664-302X
• DOI: 10.3389/fmicb.2017.01708

Environmental toxicants such as 2,3,7,8-tetrachlorodibenzo- -dioxin (TCDD), an aryl hydrocarbon receptor (AhR), are known to induce host toxicity and structural shifts in the gut microbiota. Key bacterial populations with similar or opposing functional responses to AhR ligand exposure may potentially help regulate expression of genes associated with immune dysfunction. To examine this question and the mechanisms for AhR ligand-induced bacterial shifts, C57BL/6 gnotobiotic mice were colonized with and without segmented filamentous bacteria (SFB) - an immune activator. Mice were also colonized with polysaccharide A producing - an immune suppressor to serve as a commensal background. Following colonization, mice were administered TCDD (30 μg/kg) every 4 days for 28 days by oral gavage. Quantified with the nCounter mouse immunology panel, opposing responses in ileal gene expression (e.g., genes associated with T-cell differentiation via the class II major histocompatibility complex) as a result of TCDD dosing and SFB colonization were observed. Genes that responded to TCDD in the presence of SFB did not show a significant response in the absence of SFB, and vice versa. Regulatory T-cells examined in the mesenteric lymph-nodes, spleen, and blood were also less impacted by TCDD in mice colonized with SFB. TCDD-induced shifts in abundance of SFB and compared with previous studies in mice with a traditional gut microbiome. With regard to the mouse model colonized with individual populations, results indicate that TCDD-induced host response was significantly modulated by the presence of SFB in the gut microbiome, providing insight into therapeutic potential between AhR ligands and key commensals.