Myeloid differentiation primary response gene (MyD) 88 signalling is not essential for intestinal fibrosis development

Lutz, Christian; Weder, Bruce; Hünerwadel, A.; Fagagnini, Stefania; Lang, Brian M.; Beerenwinkel, Niko; Rossel, Jean‐Benoît; Rogler, Gerhard; Misselwitz, Benjamin; Hausmann, Martin

doi:10.1038/s41598-017-17755-7

Cited by 6 publications

(8 citation statements)

References 72 publications

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“…The exact cause for the initiation and progression of fibrosis in the heterotopic intestinal transplant model is unknown. Graft rejection, ischemia, hypoxia, increased Hif1α and neo-vascularisation could contribute to fibrosis in this animal model 32 , 40 . An excessive synthesis of ECM and activation of intestinal myofibroblasts positive for both vimentin and αSMA, hallmarks in the development of fibrosis, are detectable in the heterotopic transplant animal model of intestinal fibrosis 32 , 41 .…”

Section: Discussionmentioning

confidence: 83%

“…The immune response to grafts most probably is strain specific. Previously, we observed an increase in neutrophils in the heterotopic transplantation model that may be affected by the immune response to intestinal grafts, rejection, ischemia or hypoxia, which contributes to fibrosis in the animal model but not necessarily to fibrosis in IBD patients 40 . Differences in the microbiome are likely to influence the development of intestinal fibrosis.…”

Section: Discussionmentioning

confidence: 85%

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Severity of local inflammation does not impact development of fibrosis in mouse models of intestinal fibrosis

Hünerwadel

Fagagnini

Rogler

et al. 2018

Sci Rep

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Intestinal fibrosis is thought to be a consequence of excessive tissue repair, and constitutes a common problem in patients with Crohn’s disease (CD). While fibrosis seems to require inflammation as a prerequisite it is unclear whether the severity or persistence of inflammation influences the degree of fibrosis. Our aim was to investigate the role of sustained inflammation in fibrogenesis. For the initiation of fibrosis in vivo the models of Il10−/− spontaneous colitis, dextran sodium sulfate (DSS)-induced chronic colitis and heterotopic transplantation were used. In Il10−/− mice, we determined a positive correlation between expression of pro-inflammatory factors (Il1β, Tnf, Ifnγ, Mcp1 and Il6). We also found a positive correlation between the expression of pro-fibrotic factors (Col3a1 Col1a1, Tgfβ and αSma). In contrast, no significant correlation was determined between the expression of pro-inflammatory Tnf and pro-fibrotic αSma, Col1a1, Col3a1, collagen layer thickness and the hydroxyproline (HYP) content. Results from the DSS-induced chronic colitis model confirmed this finding. In the transplantation model for intestinal fibrosis a pronounced increase in Mcp1, inos and Il6 in Il10−/− as compared to WT grafts was observed, indicating more severe inflammation in Il10−/− grafts. However, the increase of collagen over time was virtually identical in both Il10−/− and WT grafts. Severity of inflammation during onset of fibrogenesis did not correlate with collagen deposition. Although inflammation might be a pre-requisite for the initiation of fibrosis our data suggest that it has a minor impact on the progression of fibrosis. Our results suggest that development of fibrosis and inflammation may be disconnected. This may be important for explaining the inefficacy of anti-inflammatory treatments agents in most cases of fibrotic inflammatory bowel diseases (IBD).

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Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 85%

Severity of local inflammation does not impact development of fibrosis in mouse models of intestinal fibrosis

Hünerwadel

Fagagnini

Rogler

et al. 2018

Sci Rep

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“…However, bacterial translocation and the pathogen associated molecular pattern [PAMP]-associated signalling is not a prerequisite of fibrosis in this model, as collagen deposition is also increased following transplantation of small bowel from germ-free mice and MyD88-deficient mice. 56 In the heterotopic transplant model, fibrosis is also observed in the absence of B and T cells in RAG2-deficient mice [M. Hausmann, unpublished observations].…”

Section: Discussionmentioning

confidence: 99%

The Oxysterol Synthesising Enzyme CH25H Contributes to the Development of Intestinal Fibrosis

Raselli

Wyss

Alvarado

et al. 2019

Journal of Crohn's and Colitis

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Intestinal fibrosis and stenosis are common complications of Crohn’s disease [CD], frequently requiring surgery. Anti-inflammatory strategies can only partially prevent fibrosis; hence, anti-fibrotic therapies remain an unmet clinical need. Oxysterols are oxidised cholesterol derivatives with important roles in various biological processes. The enzyme cholesterol 25-hydroxylase [CH25H] converts cholesterol to 25-hydroxycholesterol [25-HC], which modulates immune responses and oxidative stress. In human intestinal samples from CD patients, we found a strong correlation of CH25H mRNA expression with the expression of fibrosis markers. We demonstrate reduced intestinal fibrosis in mice deficient for the CH25H enzyme, using the sodium dextran sulphate [DSS]-induced chronic colitis model. Additionally, using a heterotopic transplantation model of intestinal fibrosis, we demonstrate reduced collagen deposition and lower concentrations of hydroxyproline in CH25H knockouts. In the heterotopic transplant model, CH25H was expressed in fibroblasts. Taken together, our findings indicate an involvement of oxysterol synthesis in the pathogenesis of intestinal fibrosis.

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“…These data reinforce the opportunities for interferences at the regulatory and inhibitory levels. For the acute initiation or progression phases of IBD, the roles of p38 kinase and nuclear factor κB (NFκB) in breakdown of the intestinal barrier by substrate cleavage through MMP-9 ( vide supra ) have been reinforced ( 45 , 47 ). In the chronic phase, when fibrosis is happening, the toll-like receptor (TLR) system with MyD88 as transducer towards the NFκB pathway seems not essential ( 47 ).…”

Section: Insights Into Mechanisms Of Regulation Of Mmp-9 and Therapeu...mentioning

confidence: 99%

How to place the duality of specific MMP-9 inhibition for treatment of inflammatory bowel diseases into clinical opportunities?

2022

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Crohn’s disease (CD) and ulcerative colitis (UC) are inflammatory bowel diseases (IBD) with the involvement of immune cells and molecules, including cytokines, chemokines and proteases. A previous extensive review about the molecular biology of matrix metalloproteases (MMPs) and tissue inhibitors of metalloproteases (TIMPs), related to intestinal barrier destruction and restoration functions in IBD, is here complemented with the literature from the last five years. We also compare IBD as a prototypic mucosal inflammation of an epithelial barrier against microorganisms with inflammatory retinopathy as a disease with a barrier dysfunction at the level of blood vessels. Multiple reasons are at the basis of halting clinical trials with monoclonal antibodies against MMP-9 for IBD treatment. These include (i) the absence of a causative role of MMP-9 in the pathology in animal models of IBD, (ii) the fact that endotoxins, crossing the intestinal barrier, induce massive local release of both neutrophil collagenase (MMP-8) and gelatinase B (MMP-9), (iii) insufficient recognition that MMPs modify the activities of cytokines, chemokines and their receptors, (iv) ignorance that MMPs exist as mixtures of proteoforms with different posttranslational modifications and with different specific activities and (v) the fact that MMPs and TIMPs act in an interactive network, possibly having also beneficial effects on IBD evolution. Nevertheless, inhibition of MMPs may be a useful therapeutic approach during specific IBD disease phases or in specific sub-phenotypes. This temporary “window of opportunity” for MMP-9 inhibition may be complemented by a locoregional one, provided that the pharmacological agents are targeted in time to affected tissues, as is achieved in ophthalmological inflammation. Thus, in order to discover spatial and temporal windows of opportunity for MMP inhibition as treatment of IBD, more preclinical work including well controlled animal studies will be further needed. In this respect, MMP-9/NGAL complex analysis in various body compartments is helpful for better stratification of IBD patients who may benefit from anti-MMP-9.

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Myeloid differentiation primary response gene (MyD) 88 signalling is not essential for intestinal fibrosis development

Cited by 6 publications

References 72 publications

Severity of local inflammation does not impact development of fibrosis in mouse models of intestinal fibrosis

Severity of local inflammation does not impact development of fibrosis in mouse models of intestinal fibrosis

The Oxysterol Synthesising Enzyme CH25H Contributes to the Development of Intestinal Fibrosis

How to place the duality of specific MMP-9 inhibition for treatment of inflammatory bowel diseases into clinical opportunities?

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