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转化生长因子-β和配方奶喂养对易过敏大鼠饮食中β-乳球蛋白全身免疫反应的影响。

Effects of transforming growth factor-beta and formula feeding on systemic immune responses to dietary beta-lactoglobulin in allergy-prone rats.

作者信息

Penttila Irmeli

机构信息

Child Health Research Institute, North Adelaide, South Australia, Australia 5006.

出版信息

Pediatr Res. 2006 May;59(5):650-5. doi: 10.1203/01.pdr.0000203149.75465.74.

DOI:10.1203/01.pdr.0000203149.75465.74
PMID:16627876
Abstract

Early nutritional events have the potential to affect health outcomes in later life including the development of allergy. Food allergy is usually the first manifestation of allergy. Breast-feeding has been associated with a protective effect against the development of allergy, but the evidence is contradictory and the mechanisms involved are not clear. We hypothesize that milk cytokines, such as transforming growth factor beta (TGF-beta), play a role in regulating immune responses to dietary antigens. Using a rat pup model of gastrostomy feeding, the immune response profile, at weaning and post-weaning, of allergy-prone Brown Norway rats fed formula supplementation with TGF-beta was assessed. We show that feeding formula to allergy-prone rat pups results in increased total IgE immunoglobulin, beta-lactoglobulin (BLG) IgG1 antibody, and mucosal mast cell activation, as measured by serum rat mast cell protease II (RMCPII) levels in the gut. Supplementation of formula with physiological levels of TGF-beta down-regulated the BLG IgG1 response as well as total IgE and mucosal mast cell activation. Supplementation of formula also resulted in an increase in Th1 cytokines, interleukin (IL)-18, IL-12p40, IL-12p35, and interferon gamma (IFN-gamma) and an increase in IL-10. In conclusion, TGF-beta supplementation of formula moved the immune response profile of allergy prone (Th2 type) rat pups toward a Th1 profile in the suckling period. Importantly, this immune profile persisted after weaning when TGF-beta was no longer present in the diet.

摘要

早期营养事件有可能影响晚年的健康结果,包括过敏的发生。食物过敏通常是过敏的首发表现。母乳喂养与预防过敏的发生具有保护作用相关,但证据相互矛盾,且涉及的机制尚不清楚。我们推测,牛奶细胞因子,如转化生长因子β(TGF-β),在调节对饮食抗原的免疫反应中起作用。使用胃造口喂养的大鼠幼崽模型,评估了补充TGF-β配方奶喂养的易过敏棕色挪威大鼠在断奶时和断奶后的免疫反应谱。我们发现,给易过敏的大鼠幼崽喂食配方奶会导致总IgE免疫球蛋白、β-乳球蛋白(BLG)IgG1抗体增加,以及肠道黏膜肥大细胞活化,这可通过肠道中血清大鼠肥大细胞蛋白酶II(RMCPII)水平来衡量。用生理水平的TGF-β补充配方奶可下调BLG IgG1反应以及总IgE和黏膜肥大细胞活化。补充配方奶还导致Th1细胞因子、白细胞介素(IL)-18、IL-12p40、IL-12p35和干扰素γ(IFN-γ)增加,以及IL-10增加。总之,在哺乳期,用TGF-β补充配方奶使易过敏(Th2型)大鼠幼崽的免疫反应谱向Th1谱转变。重要的是,断奶后当饮食中不再存在TGF-β时,这种免疫谱仍然持续存在。

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