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在断奶期的特定阶段用益生菌约氏乳杆菌NCC533(La1)进行口服治疗,可预防NC/Nga模型小鼠成熟后诱发的特应性皮炎的发展。

Oral treatment with probiotic Lactobacillus johnsonii NCC533 (La1) for a specific part of the weaning period prevents the development of atopic dermatitis induced after maturation in model mice, NC/Nga.

作者信息

Inoue R, Nishio A, Fukushima Y, Ushida K

机构信息

Laboratory of Animal Science, Kyoto Prefectural University, Shimogamo, Kyoto, Japan.

出版信息

Br J Dermatol. 2007 Mar;156(3):499-509. doi: 10.1111/j.1365-2133.2006.07695.x.

Abstract

BACKGROUND

The inhibitory effect of probiotic bacteria on atopic dermatitis has been shown in human infants, but the mechanism is still unclear.

OBJECTIVE

This study aimed to show the effects of the administration of a probiotic during the weaning period in mouse models on production of the intestinal secretory IgA (sIgA) and on the development of atopic dermatitis (AD) in later life.

METHODS

The effects of the administration of Lactobacillus johnsonii NCC533 (La1) during weaning were evaluated using a mouse model (Balb/c). The weaning period of mice was divided into three phases according to the evolution of faecal IgA. La1 was administered in each phase and the evolution of the faecal IgA was estimated. In the next experiment, the effect of the administration of La1 in phase 2 on host immunity after maturation was further assessed by using the model NC/Nga mouse for human AD.

RESULTS

Administration of La1 in each phase showed a distinct effect on the production of sIgA. But sIgA production was only positively stimulated when La1 was administrated in phase 2. The development of AD induced by mite antigen from 6 weeks old was significantly prevented by the primary administration of La1 in phase 2. AD-like lesions were significantly milder than those of the control mice, and histological observations showed an almost normal appearance of the epidermis and upper dermis of the mice treated with La1.

CONCLUSION

This study suggested that the primary administration of La1 in a specific part of the weaning period is effective in preventing or inhibiting the development of AD after maturation by modulating or accelerating the gut immune response.

摘要

背景

益生菌对人类婴儿特应性皮炎的抑制作用已得到证实,但机制仍不清楚。

目的

本研究旨在表明在小鼠模型的断奶期给予益生菌对肠道分泌型IgA(sIgA)产生及后期特应性皮炎(AD)发展的影响。

方法

使用小鼠模型(Balb/c)评估断奶期给予约氏乳杆菌NCC533(La1)的效果。根据粪便IgA的变化将小鼠断奶期分为三个阶段。在每个阶段给予La1,并评估粪便IgA的变化。在接下来的实验中,通过使用人类AD模型NC/Nga小鼠进一步评估在第2阶段给予La1对成熟后宿主免疫的影响。

结果

在每个阶段给予La1对sIgA的产生均显示出明显影响。但仅在第2阶段给予La1时sIgA产生受到正向刺激。在第2阶段初次给予La1可显著预防6周龄时由螨抗原诱导的AD发展。AD样病变明显比对照小鼠轻,组织学观察显示用La1处理的小鼠表皮和真皮上层外观几乎正常。

结论

本研究表明在断奶期的特定阶段初次给予La1可通过调节或加速肠道免疫反应有效预防或抑制成熟后AD的发展。

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