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通过工程改造的干酪乳杆菌将牛β-乳球蛋白组成性递送至无菌小鼠的消化道。

Constitutive delivery of bovine beta-lactoglobulin to the digestive tracts of gnotobiotic mice by engineered Lactobacillus casei.

作者信息

Hazebrouck S, Oozeer R, Adel-Patient K, Langella P, Rabot S, Wal J-M, Corthier G

机构信息

Unité d'Immuno-Allergie Alimentaire, INRA-CEA, CEA de Saclay, SPI-Bât. 136, 91191 Gif-sur-Yvette cedex, France.

出版信息

Appl Environ Microbiol. 2006 Dec;72(12):7460-7. doi: 10.1128/AEM.01032-06. Epub 2006 Sep 22.

DOI:10.1128/AEM.01032-06
PMID:16997983
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1694238/
Abstract

The gut microbiota is critical for maturation of the immune system. Recent evidence suggests that early establishment of lactobacilli in the intestinal microbiota, during neonatal colonization or by probiotic supplementation, could prevent the development of allergic disorders. Postnatal maturation of the gut immune system with allergen-producing lactobacilli colonizing the digestive tract could then affect the development of further allergic sensitization. In this paper, we describe construction of a recombinant Lactobacillus casei strain that can constitutively deliver bovine beta-lactoglobulin (BLG), a major cow's milk allergen, to the guts of gnotobiotic mice. The blg gene was inserted into the L. casei chromosome downstream of an endogenous promoter. BLG production was improved by fusing the propeptide LEISSTCDA (LEISS) to the BLG mature moiety. This led to a 10-fold increase in LEISS-BLG production compared to the production obtained without the propeptide and also led to enhanced secretion corresponding to 5% of the total production. After inoculation into germfree C3H/HeN mice, the genetic stability of the recombinant strain and in vivo BLG production were confirmed for at least 10 weeks. BLG stimulation of spleen cells from mice monoassociated with the BLG-producing lactobacilli induced secretion of the Th1 cytokine gamma interferon and, to a lesser extent, the Th2 cytokine interleukin-5. No BLG-specific immunoglobulin G1 (IgG1), IgG2a, or IgA was detected in sera or in fecal samples. These results suggest that gut colonization with allergen-producing lactobacilli could provide a useful model for studying the modulation of allergic disorders.

摘要

肠道微生物群对免疫系统的成熟至关重要。最近的证据表明,在新生儿定植期间或通过补充益生菌,使乳酸菌在肠道微生物群中早期定植,可预防过敏性疾病的发生。随后,随着产生过敏原的乳酸菌在消化道定植,肠道免疫系统的产后成熟可能会影响进一步过敏致敏的发展。在本文中,我们描述了一种重组干酪乳杆菌菌株的构建,该菌株能够持续地将主要的牛奶过敏原牛β-乳球蛋白(BLG)递送至无菌小鼠的肠道。将blg基因插入内源性启动子下游的干酪乳杆菌染色体中。通过将前肽LEISSTCDA(LEISS)与BLG成熟部分融合,提高了BLG的产量。与未使用前肽时相比,这使得LEISS-BLG的产量增加了10倍,并且还导致分泌增强,相当于总产量的5%。接种到无菌C3H/HeN小鼠体内后,重组菌株的遗传稳定性和体内BLG产量在至少10周内得到了证实。用产生BLG的乳酸菌单联的小鼠脾脏细胞经BLG刺激后,诱导了Th1细胞因子γ干扰素的分泌,并在较小程度上诱导了Th2细胞因子白细胞介素-5的分泌。在血清或粪便样本中未检测到BLG特异性免疫球蛋白G1(IgG1)、IgG2a或IgA。这些结果表明,用产生过敏原的乳酸菌进行肠道定植可为研究过敏性疾病的调节提供一个有用的模型。

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