The Microbiome Activates CD4 T-cell-mediated Immunity to Compensate for Increased Intestinal Permeability

Karen L Edelblum; Gil Sharon; Gurminder Singh; Matthew A Odenwald; Anne Sailer; Severine Cao; Sarina Ravens; Irene Thomsen; Kamal El Bissati; Rima McLeod; Chen Dong; Sandeep Gurbuxani; Immo Prinz; Sarkis K Mazmanian; Jerrold R Turner

doi:10.1016/j.jcmgh.2017.06.001

The Microbiome Activates CD4 T-cell-mediated Immunity to Compensate for Increased Intestinal Permeability

Cell Mol Gastroenterol Hepatol. 2017 Jun 10;4(2):285-297. doi: 10.1016/j.jcmgh.2017.06.001. eCollection 2017 Sep.

Authors

Karen L Edelblum^{1

2}, Gil Sharon³, Gurminder Singh^{2

4}, Matthew A Odenwald², Anne Sailer², Severine Cao², Sarina Ravens⁵, Irene Thomsen⁵, Kamal El Bissati^{6

7}, Rima McLeod^{6

7}, Chen Dong⁸, Sandeep Gurbuxani², Immo Prinz⁵, Sarkis K Mazmanian³, Jerrold R Turner^{2

4}

Affiliations

¹ Department of Pathology and Laboratory Medicine, Rutgers New Jersey Medical School, Newark, New Jersey.
² Department of Pathology, University of Chicago, Chicago, Illinois.
³ Division of Biology and Biological Engineering, California Institute of Technology, Pasadena, California.
⁴ Departments of Pathology and Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts.
⁵ Institute of Immunology, Hannover Medical School, Hannover, Germany.
⁶ Department of Ophthalmology and Visual Sciences, University of Chicago, Chicago, Illinois.
⁷ Department of Pediatrics, University of Chicago, Chicago, Illinois.
⁸ Institute for Immunology, Tsinghua University, Beijing, China.

Abstract

Background & aims: Despite a prominent association, chronic intestinal barrier loss is insufficient to induce disease in human subjects or experimental animals. We hypothesized that compensatory mucosal immune activation might protect individuals with increased intestinal permeability from disease. We used a model in which intestinal barrier loss is triggered by intestinal epithelial-specific expression of constitutively active myosin light chain kinase (CA-MLCK). Here we asked whether constitutive tight junction barrier loss impacts susceptibility to enteric pathogens.

Methods: Acute or chronic Toxoplasma gondii or Salmonella typhimurium infection was assessed in CA-MLCK transgenic or wild-type mice. Germ-free mice or those lacking specific immune cell populations were used to investigate the effect of microbial-activated immunity on pathogen translocation in the context of increased intestinal permeability.

Results: Acute T gondii and S typhimurium translocation across the epithelial barrier was reduced in CA-MLCK mice. This protection was due to enhanced mucosal immune activation that required CD4⁺ T cells and interleukin 17A but not immunoglobulin A. The protective mucosal immune activation in CA-MLCK mice depended on segmented filamentous bacteria (SFB), because protection against early S typhimurium invasion was lost in germ-free CA-MLCK mice but could be restored by conventionalization with SFB-containing, not SFB-deficient, microbiota. In contrast, chronic S typhimurium infection was more severe in CA-MLCK mice, suggesting that despite activation of protective mucosal immunity, barrier defects ultimately result in enhanced disease progression.

Conclusions: Increased epithelial tight junction permeability synergizes with commensal bacteria to promote intestinal CD4⁺ T-cell expansion and interleukin 17A production that limits enteric pathogen invasion.

Keywords: Barrier Function; CA-MLCK, constitutively active myosin light chain kinase; CD4 T Cell; CFU, colony-forming unit; GF, germ-free; IL, interleukin; Ig, immunoglobulin; LP, lamina propria; Microbiota; Mucosal Immunity; SEM, standard error of the mean; SFB, segmented filamentous bacteria; SPF, specific pathogen–free; Salmonella; Tight Junction; WT, wild-type.

Abstract

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