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Elicitation of an allergic reaction in mice orally sensitized to whey or casein proteins

Published online by Cambridge University Press:  12 May 2008

A. J. Nauta ,
B. Schouten ,
B. C. A. M. van Esch ,
S. van Doorn ,
G. A. Hofman ,
L. W. J. van den Elsen ,
L. E. M. Willemsen ,
L. M. J. Knippels  and
J. Garssen
A. J. Nauta
Affiliation:
Immunology, Numico-Research BV, Wageningen, The Netherlands
B. Schouten
Affiliation:
Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
B. C. A. M. van Esch
Affiliation:
Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
S. van Doorn
Affiliation:
Immunology, Numico-Research BV, Wageningen, The Netherlands
G. A. Hofman
Affiliation:
Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
L. W. J. van den Elsen
Affiliation:
Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
L. E. M. Willemsen
Affiliation:
Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
L. M. J. Knippels
Affiliation:
Immunology, Numico-Research BV, Wageningen, The Netherlands
J. Garssen
Affiliation:
Immunology, Numico-Research BV, Wageningen, The Netherlands Pharmacology and Pathophysiology, UIPS, Utrecht University, The Netherlands
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Abstract

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Type
1st International Immunonutrition Workshop, Valencia, 3–5 October 2007, Valencia, Spain
Information
Proceedings of the Nutrition Society , Volume 67 , Issue OCE1: 1st International Immunonutrition Workshop, Valencia, 3–5 October 2007, Valencia, Spain , May 2008 , E57
Copyright
Copyright © The Authors 2008

Cow's-milk allergy (CMA) is the most common food allergy in children, affecting 1–2% of all infants. So far, the pathogenesis of the disease is incompletely understood, and no effective treatment is available to cure or actively prevent food allergy. Animal models may provide a useful tool to explore the mechanisms underlying the development of CMA and to identify new therapeutic strategies. The purpose of the present study was to develop a murine model of IgE-mediated cow's milk hypersensitivity that closely mimics the clinical features of human CMA.

Female C3H/HeOuJ mice (5 weeks old; n 6) were sensitized by intragastric administration of casein or whey, using cholera toxin (CT) as an adjuvant (methods adapted from Li et al. 1999 and Frossard et al. 2004(Reference Frossard, Hauser and Eigenmann1, Reference Li, Schofield, Huang, Kleiner and Sampson2)) and boosted five times at weekly intervals. At week 7 the mice were challenged subcutaneously (ear) and orally. Serum levels of mouse mast cell protease-1 (mMCP-1), total IgE and allergen-specific IgE, IgG1 and IgG2a were measured. The acute allergic skin reaction was determined by measuring ear swelling.

An antigen-specific acute allergic skin response was induced in casein- and whey-sensitized mice (μm; 71.2 (sd 8.4) and 137.9 (sd 21.7) respectively v. −4.6 (sd 4.7) for CT controls; P<0.01). Total IgE and mMCP-1 serum concentrations were enhanced in both the casein- and whey-sensitized mice. In whey-sensitized mice whey-specific IgE, IgG1 and IgG2a serum levels were enhanced, while in casein-sensitized mice only casein-specific IgG1 was increased (Table). In casein-sensitized mice the number of mast cells per villus–crypt unit was enhanced compared with whey-sensitized and CT control mice (1.0 (sd 0.2) v. 0.1 (sd 0.1) v. 0.3 (sd 0.0); P<0.01).

Taken together these results suggest that the oral administration of whey and casein elicit an allergic reaction in mice that mimics immediate CMA in human subjects. Differential pathophysiological changes were observed in whey-sensitized and casein-sensitized mice. The serology of whey-sensitized mice more closely resembles the human situation, whereas casein-sensitized mice develop gastrointestinal symptoms similar to the clinical features of human CMA. These mouse models of CMA provide a useful tool to examine the mechanism underlying the development of CMA and to explore new therapeutic strategies for the treatment of food allergy.

* Presented as OD values.

References

1. Frossard, CP, Hauser, C & Eigenmann, PA (2004) J Allergy Clin Immunol 114, 377382.CrossRefGoogle Scholar
2. Li, XM, Schofield, BH, Huang, CK, Kleiner, GI & Sampson, HA (1999) J Allergy Clin Immunol 103, 206214.Google Scholar