Differential Requirements for IL-17A and IL-22 in Cecal versus Colonic Inflammation Induced by Helicobacter hepaticus

Morrison, Peter J; Ballantyne, Sarah J.; MacDonald, Sandy; Moore, John W. J.; Jenkins, D. G.; Wright, Jill F.; Fouser, Lynette A.; Kullberg, Marika C.

doi:10.1016/j.ajpath.2015.08.015

Cited by 18 publications

(14 citation statements)

References 55 publications

(66 reference statements)

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“…whereas, anti-Il-17 treatment increased severity of cecal pathology but not colonic pathology (Kullberg et al, 2006;Morrison et al, 2015). Thus, it is possible that the progression of preneoplastic dysplasia to cancer promoted by HhCDT requires a host factor(s) and a defined microflora only present in the ceca and ileocecocoloic junction.…”

Section: Stat3 Can Be Activated By Diverse Agents Including Growth Famentioning

confidence: 83%

“…Consistent with these previous findings, in the Hh‐infected mice, there was more severe pathology in the ceca and ileocecocolic junction compared with transverse and distal colon at both time points and in the HhCDT mutant‐infected mice at 10 WPI. In addition, previous studies in anti‐Il10R‐treated C57BL/6 mice reported that Il‐22 and Ifnγ are required for inducing colonic inflammation but not for cecal inflammation by H. hepaticus ; whereas, anti‐Il‐17 treatment increased severity of cecal pathology but not colonic pathology (Kullberg et al, ; Morrison et al, ). Thus, it is possible that the progression of preneoplastic dysplasia to cancer promoted by HhCDT requires a host factor(s) and a defined microflora only present in the ceca and ileocecocoloic junction.…”

Section: Discussionmentioning

confidence: 95%

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Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

Feng

et al. 2017

Cellular Microbiology

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Summary Multiple pathogenic Gram-negative bacteria produce the cytolethal distending toxin (CDT) with activity of DNase I; CDT can induce DNA double strand breaks (DSBs), G2/M cell cycle arrest and apoptosis in cultured mammalian cells. However, the link of CDT to in vivo tumorigenesis is not fully understood. In this study, 129/SvEv Rag2−/− mice were gavaged with wild-type Helicobacter hepatics 3B1(Hh) and its isogenic cdtB mutant HhcdtBm7, followed by infection for 10 and 20 weeks (WPI). HhCDT-deficiency did not affect cecal colonization levels of HhcdtBm7, but attenuated severity of cecal pathology in HhcdtBm7-infected mice. Of importance, preneoplasic dysplasia was progressed to cancer from 10 WPI to 20 WPI in the Hh-infected mice but not in the HhcdtBm7-infected mice. In addition, the loss of HhCDT significantly dampened transcriptional upregulation of cecal Tnfα and Il-6, but elevated Il-10 mRNA levels when compared to Hh at 10 WPI. Furthermore, the presence of HhCDT increased numbers of lower bowel intestinal γH2AX-positive epithelial cells (a marker of DSBs) at both 10 WPI and 20 WPI, and augmented phospho-Stat3 foci+ intestinal crypts (activation of Stat3) at 20 WPI. Our findings suggest that CDT promoted Hh carcinogenesis by enhancing DSBs and activation of the Tnfα /Il-6-Stat3 signaling pathway.

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Section: Stat3 Can Be Activated By Diverse Agents Including Growth Famentioning

confidence: 83%

Section: Discussionmentioning

confidence: 95%

Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

Feng

et al. 2017

Cellular Microbiology

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“…In our study, there were no differences in the cecum typhlocolitis index scores between genders, but the female mice had significantly higher pathological scores in the colon at both 6 and 10 weeks p.i. The underlying differences in the expression of cytokine receptors in different anatomical locations of the intestine may contribute to this difference (39). At 6 weeks p.i, multifocal hepatitis was noticed in the infected mice which may indicate H.japonicum infection in the liver by translocating the intestinal barrier into hepatic tissues or alternatively, indirect effect of systemic cytokine response due to the primary intestinal infection (40).…”

Section: Discussionmentioning

confidence: 99%

NovelHelicobacterspeciesH.japonicumisolated from laboratory mice from Japan induces typhlocolitis and lower bowel carcinoma in C57BL/129 IL10^−/−mice

Shen¹,

Feng²,

Muthupalani³

et al. 2016

CARCIN

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A novel Helicobacter species Helicobacter japonicum was isolated from the stomach and intestines of clinically normal mice received from three institutes from Japan. The novel Helicobacter sp. was microaerobic, grew at 37°C and 42°C, was catalase and oxidase positive, but urease negative. It is most closely related to the 16S rRNA gene of H.muridarum (98.6%); to the 23S rRNA gene of H.hepaticus (97.9%); to the hsp60 gene of H.typhlonius (87%). The novel Helicobacter sp. has in vitro cytolethal distending toxin (CDT) activity; its cdtB gene sequence has 83.8% identity with that of H.hepaticus. The whole genome sequence of H.japonicum MIT 01-6451 has a 2.06-Mb genome length with a 37.5% G + C content. When the organism was inoculated into C57BL/129 IL10 −/− mice, it was cultured from the stomach, colon and cecum of infected mice at 6 and 10 weeks post-infection. The cecum had the highest H.japonicum colonization levels by quantitative PCR. The histopathology of the lower bowel was characterized by moderate to severe inflammation, mild edema, epithelial defects, mild to severe hyperplasia, dysplasia and carcinoma. Inflammatory cytokines IFNγ, TNFα and IL17a, as well as iNOS were significantly upregulated in the cecal tissue of infected mice. These results demonstrate that the novel H.japonicum can induce inflammatory bowel disease and carcinoma in IL10 −/− mice and highlights the importance of identifying novel Helicobacter spp. especially when they are introduced from outside mouse colonies from different geographic locations.

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“…H. hepaticus‐ or H. typhlonius ‐infected mice are frequently used as a model for a better understanding of the pathogenesis of inflammatory bowel diseases in humans. IL‐23 produced by monocytes, IL‐17 and IL‐22 produced by Th17 cells, IFNγ and IL‐17 produced by Th1/17 cells, and TNFα produced by colitogenic T cells seem to be associated with the development of intestinal inflammation. Ray et al .…”

Section: Pathogenesis Of Infections With Nhphmentioning

confidence: 99%

Other Helicobacters and gastric microbiota

et al. 2016

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This article aimed to review the literature from 2015 dealing with gastric and enterohepatic non-Helicobacter pylori Helicobacter species (NHPH). A summary of the gastric microbiota interactions with H. pylori is also presented. An extensive number of studies were published during the last year and have led to a better understanding of the pathogenesis of infections with NHPH. These infections are increasingly reported in human patients, including infections with H. cinaedi, mainly characterized by severe bacteremia. Whole-genome sequencing appears to be the most reliable technique for identification of NHPH at species level. Presence of NHPH in laboratory animals may influence the outcome of experiments, making screening and eradication desirable. Vaccination based on UreB proteins or bacterial lysate with CCR4 antagonists as well as oral glutathione supplementation may be promising strategies to dampen the pathogenic effects associated with gastric NHPH infections. Several virulent factors such as outer membrane proteins, phospholipase C-gamma 2, Bak protein, and nickel-binding proteins are associated with colonization of the gastric mucosae and development of gastritis. The development of high-throughput sequencing has led to new insights in the gastric microbiota composition and its interaction with H. pylori. Alterations in the gastric microbiota caused by the pH-increasing effect of a H. pylori infection may increase the risk for gastric cancer.

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Differential Requirements for IL-17A and IL-22 in Cecal versus Colonic Inflammation Induced by Helicobacter hepaticus

Cited by 18 publications

References 55 publications

Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

NovelHelicobacterspeciesH.japonicumisolated from laboratory mice from Japan induces typhlocolitis and lower bowel carcinoma in C57BL/129 IL10^−/−mice

Other Helicobacters and gastric microbiota

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Differential Requirements for IL-17A and IL-22 in Cecal versus Colonic Inflammation Induced by Helicobacter hepaticus

Cited by 18 publications

References 55 publications

Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

Helicobacter hepaticuscytolethal distending toxin promotes intestinal carcinogenesis in 129Rag2-deficient mice

NovelHelicobacterspeciesH.japonicumisolated from laboratory mice from Japan induces typhlocolitis and lower bowel carcinoma in C57BL/129 IL10−/−mice

Other Helicobacters and gastric microbiota

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NovelHelicobacterspeciesH.japonicumisolated from laboratory mice from Japan induces typhlocolitis and lower bowel carcinoma in C57BL/129 IL10^−/−mice