Altered expression of tissue remodeling genes in a mouse model of acute allergic rhinitis

Sautter, Nathan B.; Delaney, Katherine L.; Trune, Dennis R.

doi:10.1002/alr.20059

Cited by 14 publications

(18 citation statements)

References 35 publications

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“…In the same test, the expression of a range of cytokines from Fibroblast Growth Factors (FGF) and Matrix Metalloproteinases (MMP) was found to be elevated after exposure to a specific allergen. These findings suggest that signal transduction in cells intended for initiating the process of fibrogenesis and remodelling is initiated earlier in inflammatory illnesses [29].…”

Section: The Bmp Protein and Bmpr Receptor: Expression Function And mentioning

confidence: 89%

Selected Bone Morphogenetic Proteins—The Possibility of Their Use in the Diagnostics and Therapy of Severe Asthma

Koćwin

Jonakowski

Przemęcka

et al. 2017

Advances in Respiratory Medicine

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Asthma is a chronic heterogeneous illness of the lower airway with an inflammatory basis, developing from hyperresponsiveness and bronchial obstruction. One of the more unfavourable processes occurring in the airway are the long-term changes of the respiratory tract known as remodelling, resulting in complete irreversible obstruction. Bone morphogenetic protein (BMP) is a member of the Transforming Growth Factor beta (TGF-b) superfamily, which regulates processes in embryonic and post-embryonic development. The role played by BMP is regulation of degradation and remodelling of the extracellular matrix, which is one of the elements involved in the reconstruction of the structure of the bronchi in severe asthma. This paper presents the antagonistic properties of BMP against TGF-b, anti-inflammatory and counteracting fibrosis in the respiratory tract. The current state of knowledge indicates that this group of cytokines are potential new markers of remodelling in severe asthma, and further studies on their therapeutic value are necessary.

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Section: The Bmp Protein and Bmpr Receptor: Expression Function And mentioning

confidence: 89%

Selected Bone Morphogenetic Proteins—The Possibility of Their Use in the Diagnostics and Therapy of Severe Asthma

Koćwin

Jonakowski

Przemęcka

et al. 2017

Advances in Respiratory Medicine

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“…Quantitation of the amount of target in samples is done by measuring C t and using the standard curve to determine starting copy number. Calculation of C t s, preparation of a standard curve, determination of the starting copy number, and calculation of statistical significance was performed using the ΔΔC t method with the aid of the SABiosciences PCR Array Data Analysis Web Portal 22. 18S RNA was used as the comparator.…”

Section: Methodsmentioning

confidence: 99%

“…A better understanding of the cellular and molecular processes leading to osteogenesis, fibrosis, and angiogenesis in CRS is needed in order to develop novel therapies aimed at halting or reversing CRS‐associated tissue remodeling. We have previously demonstrated acute changes in several members of the BMP, FGF, and MMP families in a mouse model of acute allergic rhinitis 22. The purpose of this study is to characterize the changes in BMP, FGF, and MMP family expression in a mouse model of CRS.…”

Section: Introductionmentioning

confidence: 96%

Tissue remodeling gene expression in a murine model of chronic rhinosinusitis

et al. 2012

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Objective/Hypothesis The Matrix Metalloproteinase (MMP), Fibroblast Growth Factor (FGF) and Bone Morphogenetic Protein (BMP) families regulate tissue remodeling in many normal and pathophysiologic processes. We hypothesize that induction of chronic sinonasal inflammation will be associated with changes in regulation of these tissue remodeling cytokines. Methods Balb/c mice aged 8–12 weeks were sensitized and treated with intranasal Aspergillus fumigatis (AF) three times per week for 1 week, 3 weeks, 2 months and 3 months (n=8 each time point). Sinonasal tissues were evaluated for changes in MMP, FGF and BMP regulation using standard RT-PCR techniques. Additional snouts were processed for histology and immunohistochemistry. Untreated mouse snouts of identical age were used as controls. Results Significant upregulation of MMP8 was observed at 2 months, and MMP1a, MMP7, MMP8 and MMP12 were all significantly upregulated at 3 months. FGF3 was significantly upregulated at 3 weeks and 3 months, and FGF5, FGF6 and FGF8 were all significantly upregulated at 3 months. BMP8b and BMP9 were significantly upregulated at 3 months. Histologic analysis revealed mucosal, stromal and mucin gland hypertrophy, increased mucin production, and metaplasia with loss of cilia. Antibody staining was strongly positive in the AF treated group. Conclusion Induction of CRS is associated with time-dependent changes in tissue remodeling cytokine expression occurring in conjuction with inflammatory tissue changes. Antibody staining for upregulated cytokines suggests local production within the sinonasal mucosa. Further study is required to better understand the association between BMP, FGF and MMP regulation and tissue remodeling changes resulting from chronic inflammation.

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“…As with the ion channel genes, the general pattern of remodeling gene expression was similar in the middle ear and inner ear. Previous work has shown that these genes are indeed affected by allergic fungal rhinosinusitis and otitis media in the mouse model 3, 40 . Altered expression of these genes in the inner ear in the chronic OM model has not previously been shown.…”

Section: Discussionmentioning

confidence: 93%

Inner Ear Tissue Remodeling and Ion Homeostasis Gene Alteration in Murine Chronic Otitis Media

MacArthur¹,

Hausman²,

Kempton³

et al. 2013

Otology &Amp; Neurotology

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Hypothesis Studies were designed to ascertain the impact of chronic middle ear infection on the numerous ion and water channels, transporters and tissue remodeling genes in the inner and middle ear. Background Permanent sensorineural hearing loss is a significant problem resulting from chronic middle ear disease, although the inner ear processes involved are poorly defined. Maintaining a balanced ionic composition of endolymph in the inner ear is crucial for hearing, thus, it was hypothesized this may be at risk with inflammation. Methods Inner and middle ear RNA collected separately from 6 month-old C3H/HeJ mice with prolonged middle ear disease were subjected to qRT-PCR for 8 common inflammatory cytokine genes, 24 genes for channels controlling ion (sodium, potassium, chloride) and water (aquaporin) transport, tight junction claudins, and gap junction connexins, and 32 tissue remodeling genes. Uninfected Balb/c mice were used as controls. Results Significant increase in inner ear inflammatory and ion homeostasis (claudin, aquaporin and gap junction) gene expression, and both up- and down-regulation of tissue remodeling gene expression occurred. Alteration in middle ear ion homeostasis and tissue remodeling gene expression was noted in the setting of uniform upregulation of cytokine genes. Conclusions Chronic inflammatory middle ear disease can impact inner ear ion and water transport functions and induce tissue remodeling. Recognizing these inner ear mechanisms at risk may identify potential therapeutic targets to maintain hearing during prolonged otitis media.

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Altered expression of tissue remodeling genes in a mouse model of acute allergic rhinitis

Cited by 14 publications

References 35 publications

Selected Bone Morphogenetic Proteins—The Possibility of Their Use in the Diagnostics and Therapy of Severe Asthma

Selected Bone Morphogenetic Proteins—The Possibility of Their Use in the Diagnostics and Therapy of Severe Asthma

Tissue remodeling gene expression in a murine model of chronic rhinosinusitis

Inner Ear Tissue Remodeling and Ion Homeostasis Gene Alteration in Murine Chronic Otitis Media

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