PTPN2 regulates bacterial clearance in a mouse model of enteropathogenic and enterohemorrhagic E. coli infection
Marianne R. Spalinger, Vinicius Canale, Anica Becerra, Ali Shawki, Meli’sa Crawford, Alina N. Santos, Pritha Chatterjee, Jiang Li, Meera G. Nair, Declan F. McCole
Marianne R. Spalinger, Vinicius Canale, Anica Becerra, Ali Shawki, Meli’sa Crawford, Alina N. Santos, Pritha Chatterjee, Jiang Li, Meera G. Nair, Declan F. McCole
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Research Article Gastroenterology Inflammation

PTPN2 regulates bacterial clearance in a mouse model of enteropathogenic and enterohemorrhagic E. coli infection

Abstract

Macrophages intimately interact with intestinal epithelial cells, but the consequences of defective macrophage–epithelial cell interactions for protection against enteric pathogens are poorly understood. Here, we show that in mice with a deletion in protein tyrosine phosphatase nonreceptor type 2 (PTPN2) in macrophages, infection with Citrobacter rodentium, a model of enteropathogenic and enterohemorrhagic E. coli infection in humans, promoted a strong type 1/IL-22–driven immune response, culminating in accelerated disease but also faster clearance of the pathogen. In contrast, deletion of PTPN2 specifically in epithelial cells rendered the epithelium unable to upregulate antimicrobial peptides and consequently resulted in a failure to eliminate the infection. The ability of PTPN2-deficient macrophages to induce faster recovery from C. rodentium was dependent on macrophage-intrinsic IL-22 production, which was highly increased in macrophages deficient in PTPN2. Our findings demonstrate the importance of macrophage-mediated factors, and especially macrophage-derived IL-22, for the induction of protective immune responses in the intestinal epithelium, and show that normal PTPN2 expression in the epithelium is crucial to allow for protection against enterohemorrhagic E. coli and other intestinal pathogens.

Authors

Marianne R. Spalinger, Vinicius Canale, Anica Becerra, Ali Shawki, Meli’sa Crawford, Alina N. Santos, Pritha Chatterjee, Jiang Li, Meera G. Nair, Declan F. McCole

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Figure 4

Ptpn2ΔIEC/ERT mice have pronounced C. rodentium–induced disease.

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Ptpn2ΔIEC/ERT mice have pronounced C. rodentium–induced disease. Ptpn2Δ...
Ptpn2ΔIEC/ERT (ΔIEC/ERT) mice (5–8 weeks old) and their Ptpn2fl/fl littermates (WT) were injected with 1 mg/kg tamoxifen for 5 consecutive days. Four weeks later, the mice were infected with 5 × 108 CFU of C. rodentium. The graphs show (A) weight development, (B) disease activity, and (C) spleen weight on indicated days; C. rodentium load in (D) feces over time and in (E) liver, spleen, and mesenteric lymph nodes (mLN) at the indicated days. (F) Representative histological pictures of the distal colon at the indicated day after infection and scoring of damage and infiltration. Original magnification, 100×. (G) Il22 mRNA expression. (H) Phospho-STAT3 (pSTAT3) and total STAT3 (tSTAT3) and phospho-STAT1 (pSTAT1) and total STAT1 (tSTAT1) in the colon. (I) Reg3g, Reg3b, and Muc2 mRNA expression in the colon. Representative results from 1 of 2 experiments with n = 3–5/group; each dot represents 1 mouse. *P < 0.05 by 2-way ANOVA (A, B, and D) or Student’s 2-sided t test (C, EG, and I). Δ, change in; Ctr, control; d, day.