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Substance P antagonist improves both obesity and asthma in a mouse model

2012-11Journal article Open access
http://hdl.handle.net/10400.22/18592
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Authors

Ramalho, R.
Beltrão, M.
Pirraco, A.
Costa, R.
Sokhatska, O.
Guardão, L.
Palmares, C.
Guimarães, J. T.
Delgado, L.

Advisor(s)

Abstract(s)

Evidence suggests a causal relationship between obesity and asthma; however, the underlying mechanisms remain unknown. Substance P (SP), involved in neurogenic inflammation by acting through its receptor NK1-R, seems to participate in obese–asthma phenotype in mice. To evaluate the effect of a selective substance P receptor antagonist on a mouse model of diet-induced obesity and asthma. Diet-induced obese Balb/c mice were sensitized and challenged with ovalbumin (OVA) and treated with a selective NK1-R antagonist or placebo. Serum glucose, insulin, IL-6, resistin, and OVA-specific IgE levels were quantified. A score for peribronchial inflammation in lung histology was used. Cells were counted in bronchoalveolar lavage fluid. Adipocyte sizes were measured. Ovalbumin-obese mice treated with NK1-R antagonist had lower weight (P = 0.0002), reduced daily food intake (P = 0.0021), reduced daily energy intake (P = 0.0021), reduced surface adipocyte areas (P < 0.0001), lower serum glucose (P = 0.04), lower serum insulin (P = 0.03), lower serum IL-(P = 0.0022), lower serum resistin (P = 0.0043), lower serum OVA-specific IgE (P = 0.035), and lower peribronchial inflammation score (P < 0.0001) than nontreated OVA-obese mice. We observed an interaction between obesity, allergen sensitization, and treatment with NK1-R antagonist for metabolic and systemic biomarkers, and for allergen sensitization and bronchial inflammation, showing a synergy between these variables. In an experimental model of obesity and asthma in mice, NK1-R blockade improved metabolic and systemic biomarkers, as well as allergen sensitization and bronchial inflammation. These positive effects support a common pathway in the obese–asthma phenotype and highlight SP as a target with potential clinical interest in the obese–asthma epidemics.

Description

Keywords

Animal model Asthma NK1-R antagonist Obesity Substance P Treatment

URI

http://hdl.handle.net/10400.22/18592

Citation

Ramalho, R., Almeida, J., Beltrão, M., Pirraco, A., Costa, R., Sokhatska, O., Guardão, L., Palmares, C., Guimarães, J. T., Delgado, L., Moreira, A., & Soares, R. (2013). Substance P antagonist improves both obesity and asthma in a mouse model. Allergy, 68(1), 48-54. https://doi.org/https://doi.org/10.1111/all.12052

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Publisher

Wiley

DOI

10.1111/all.12052

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ESS - CQB - Artigos

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