BALB/c mice genetically susceptible to proteoglycan-induced arthritis and spondylitis show colony-dependent differences in disease penetrance

Farkas, Balint; Boldizsár, Ferenc; Tarjányi, Oktávia; László, Anna; Lin, Simon; Hutás, Gábor; Tryniszewska, Beáta; Mangold, Aaron R.; Nagyéri, György; Rosenzweig, Holly L.; Finnegan, Alison; Mikecz, Katalin; Glant, Tibor T.

doi:10.1186/ar2613

Cited by 20 publications

(16 citation statements)

References 89 publications

(93 reference statements)

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“…Naïve BALB/c mice rarely develop spontaneous inflammation in synovial joints (Adarichev et al, 2008; Farkas et al, 2009). BALB/c females infected with B. melitensis for 26 weeks exhibited multiple skeletal involvement with inflammatory and non-inflammatory features.…”

Section: Resultsmentioning

confidence: 99%

Osteoarticular tissue infection and development of skeletal pathology in murine brucellosis

Magnani

Lyons

Forde

et al. 2013

Disease Models &Amp; Mechanisms

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SUMMARYBrucellosis, a frequent bacterial zoonosis, can produce debilitating chronic disease with involvement of multiple organs in human patients. Whereas acute brucellosis is well studied using the murine animal model, long-term complications of host-pathogen interaction remain largely elusive. Human brucellosis frequently results in persistent, chronic osteoarticular system involvement, with complications such as arthritis, spondylitis and sacroiliitis. Here, we focused on identifying infectious sites in the mouse that parallel Brucella melitensis foci observed in patients. In vivo imaging showed rapid bacterial dispersal to multiple sites of the murine axial skeleton. In agreement with these findings, immunohistochemistry revealed the presence of bacteria in bones and limbs, and in the lower spine vertebrae of the axial skeleton where they were preferentially located in the bone marrow. Surprisingly, some animals developed arthritis in paws and spine after infection, but without obvious bacteria in these sites. The identification of Brucella in the bones of mice corroborates the findings in humans that these osteoarticular sites are important niches for the persistence of Brucella in the host, but the mechanisms that mediate pathological manifestations in these sites remain unclear. Future studies addressing the immune responses within osteoarticular tissue foci could elucidate important tissue injury mediators and Brucella survival strategies.

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Section: Resultsmentioning

confidence: 99%

Osteoarticular tissue infection and development of skeletal pathology in murine brucellosis

Magnani

Lyons

Forde

et al. 2013

Disease Models &Amp; Mechanisms

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show abstract

“…The cytokine signature is a key determining factor for developing immunomodulatory therapies for RA or other autoimmune diseases, as discussed in [60]. Determination of the Th cytokine repertoire may be complicated because different inducers and mechanisms of induction elicit different responses, and different strains of mice and even mice of the same strain from different vendors may exhibit different responses [61]. In addition, more recent literature suggests that the Th phenotype is plastic and Treg cells can convert to Th17 cells [21] and in man, Th17 cells can convert to Th1 cells, as seen at inflammatory sites such as in the synovial fluid of patients with juvenile idiopathic arthritis [62].…”

Section: Autoimmune Diseasesmentioning

confidence: 99%

Rheumatoid arthritis vaccine therapies: perspectives and lessons from therapeutic ligand epitope antigen presentation system vaccines for models of rheumatoid arthritis

Rosenthal

Mikecz

Steiner

et al. 2015

Expert Review of Vaccines

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The current status of therapeutic vaccines for autoimmune diseases is reviewed with rheumatoid arthritis as the focus. Therapeutic vaccines for autoimmune diseases must regulate or subdue responses to common self-antigens. Ideally, such a vaccine would initiate an antigen-specific modulation of the T-cell immune response that drives the inflammatory disease. Appropriate animal models and types of T helper cells and signature cytokine responses that drive autoimmune disease are also discussed. Interpretation of these animal models must be done cautiously because the means of initiation, autoantigens, and even the signature cytokine and T helper cell (Th1 or Th17) responses that are involved in the disease may differ significantly from those in humans. We describe ligand epitope antigen presentation system vaccine modulation of T-cell autoimmune responses as a strategy for the design of therapeutic vaccines for rheumatoid arthritis, which may also be effective in other autoimmune conditions.

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“…This is due to several factors including possible colony differences from different vendors and over time (Farkas et al . , 2009), differences in water intake between the studies and the large differences in study duration that potentially change the disposition of Cr(VI) over time. For example, these high concentrations of Cr(VI) can potentially alter gut microflora (Shrivastava et al .…”

Section: Application Of the Mode Of Action Frameworkmentioning

confidence: 99%

Assessment of the mode of action underlying development of rodent small intestinal tumors following oral exposure to hexavalent chromium and relevance to humans

Thompson

Proctor

Suh

et al. 2013

Critical Reviews in Toxicology

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Chronic exposure to high concentrations of hexavalent chromium (Cr(VI)) in drinking water causes intestinal adenomas and carcinomas in mice, but not in rats. Cr(VI) causes damage to intestinal villi and crypt hyperplasia in mice after only one week of exposure. After two years of exposure, intestinal damage and crypt hyperplasia are evident in mice (but not rats), as are intestinal tumors. Although Cr(VI) has genotoxic properties, these findings suggest that intestinal tumors in mice arise as a result of chronic mucosal injury. To better understand the mode of action (MOA) of Cr(VI) in the intestine, a 90-day drinking water study was conducted to collect histological, biochemical, toxicogenomic and pharmacokinetic data in intestinal tissues. Using MOA analyses and human relevance frameworks proposed by national and international regulatory agencies, the weight of evidence supports a cytotoxic MOA with the following key events: (a) absorption of Cr(VI) from the intestinal lumen, (b) toxicity to intestinal villi, (c) crypt regenerative hyperplasia and (d) clonal expansion of mutations within the crypt stem cells, resulting in late onset tumorigenesis. This article summarizes the data supporting each key event in the MOA, as well as data that argue against a mutagenic MOA for Cr(VI)-induced intestinal tumors.

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BALB/c mice genetically susceptible to proteoglycan-induced arthritis and spondylitis show colony-dependent differences in disease penetrance

Cited by 20 publications

References 89 publications

Osteoarticular tissue infection and development of skeletal pathology in murine brucellosis

Osteoarticular tissue infection and development of skeletal pathology in murine brucellosis

Rheumatoid arthritis vaccine therapies: perspectives and lessons from therapeutic ligand epitope antigen presentation system vaccines for models of rheumatoid arthritis

Assessment of the mode of action underlying development of rodent small intestinal tumors following oral exposure to hexavalent chromium and relevance to humans

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