Journal of Nutritional Science and Vitaminology
Online ISSN : 1881-7742
Print ISSN : 0301-4800
ISSN-L : 0301-4800
Further Evidence Regarding the Effect of Dietary Protein on Oral Tolerant against Beta-Lactoglobulin through Th 1-Mediated Immune Response in Mice
Sherin AHMEDMohammed A. SATTERIShigeru YAMAMOTOKen-ichi MAEDAYoshihiro MINATOFusao OTA
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JOURNAL FREE ACCESS

2003 Volume 49 Issue 2 Pages 112-119

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Abstract

Oral tolerance is a potential strategy for preventing or minimizing aberrant immune responses. Although, oral tolerance has been extensively studied, to date the effects of dietary protein on the induction of oral tolerance are poorly understood. We have previously shown that restricted dietary protein induces oral tolerance to ovalbumin. This study was designed to investigate whether or not such tolerance occurs with beta-lactoglobulin (BLG) instead of ovalbumin (OVA) and if the tolerance resulting from this feeding regimen involves Thl-mediated immune response. Female BALB/c mice fed either 20% or 5% dietary protein were given 5 mg BLG or water orally for four consecutive days and then immunized intraperitoneally (ip) twice with BLG at 3-wk intervals. Oral tolerance induction was compared in BLG-fed and water-fed mice by measuring total IgE, BLG-specific antibodies, footpad reactions, splenocyte proliferation, and cytokine production. When mice were given BLG orally before ip immunization, the Thl-mediated immune responses (production of IL-2, IFN-y, and IgG2a) were significantly reduced, whereas the Th2-mediated immune responses (production of IL-4 and IgGl) were unchanged. The Thl-mediated immune responses were markedly down-regulated in mice fed 5% protein as compared to those in mice fed 20% protein. Moreover, the production of total IgE, BLG-specific IgE, splenocyte proliferation, and footpad reactions were more reduced in mice fed 5% protein than those in mice fed 20% protein. The present study provides evidence that dietary protein plays an important role in the induction of oral tolerance against BLG as the result of, clear down-regulation of Thl helper activity accompanied by a reduction in IgE.

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