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用于炎症性肠病的益生菌的生物正交偶联和响应性纳米涂层。

Bioorthogonal conjugation and responsive nanocoating of probiotics for inflammatory bowel disease.

机构信息

Frontiers Science Center for Flexible Electronics (FSCFE), Xi'an Institute of Flexible Electronics (IFE), Xi'an Institute of Biomedical Materials and Engineering (IBME), Ningbo Institute, Northwestern Polytechnical University (NPU), Xi'an 710072, China.

Frontiers Science Center for Flexible Electronics (FSCFE), Xi'an Institute of Flexible Electronics (IFE), Xi'an Institute of Biomedical Materials and Engineering (IBME), Ningbo Institute, Northwestern Polytechnical University (NPU), Xi'an 710072, China.

出版信息

J Control Release. 2024 Oct;374:538-549. doi: 10.1016/j.jconrel.2024.08.036. Epub 2024 Aug 30.

DOI:10.1016/j.jconrel.2024.08.036
PMID:39186984
Abstract

Inflammatory bowel disease (IBD) is closely associated with dysregulated immune response, gut mucosal barrier, and microbiota. Conventional treatments suffer from inferior bioavailability and inadequate efficiency. Herein, we present a synergistic therapeutic strategy based on multifunctionalized probiotics to mitigate IBD through single oral administration. The probiotic (Escherichia coli Nissle 1917) is bioorthogonally conjugated with immunomodulators and subsequently encapsulated by an enteric coating. The viability and bioactivity of probiotics are not affected by the modifications. And the armored probiotics are able to resist the harsh environment of the stomach and shed their enteric coating in the intestinal tract, exposing immunomodulators to polarize pro-inflammatory M1-type macrophages into anti-inflammatory M2-type. In a mouse colitis model, orally administered multifunctionalized probiotics cooperatively alleviate IBD with increased body weight to 1.13 folds and decreased disease activity index to 0.43 folds, through downregulating the pro-inflammatory cytokines expression, upregulating the epithelial tight junction-associated proteins levels to restore the intestinal barrier, and increasing the microbiota richness and abundance. This work exhibits a feasible approach to construct functionalized orally administered probiotics for enhanced synergistic therapy of IBD.

摘要

炎症性肠病(IBD)与免疫反应失调、肠道黏膜屏障和微生物群密切相关。传统的治疗方法存在生物利用度低和效率不足的问题。本文提出了一种基于多功能益生菌的协同治疗策略,通过单次口服给药来减轻 IBD。该益生菌(大肠杆菌 Nissle 1917)通过生物正交反应与免疫调节剂偶联,然后被肠溶性包衣包裹。修饰过程不影响益生菌的活力和生物活性。装甲益生菌能够抵抗胃部恶劣的环境,并在肠道中脱落肠溶性包衣,使免疫调节剂将促炎 M1 型巨噬细胞极化为抗炎 M2 型。在小鼠结肠炎模型中,口服给予多功能益生菌协同治疗可使体重增加 1.13 倍,疾病活动指数降低 0.43 倍,从而减轻 IBD,其机制是通过下调促炎细胞因子的表达,上调上皮紧密连接相关蛋白的水平以恢复肠道屏障,并增加微生物群的丰富度和丰度。这项工作展示了一种构建功能性口服益生菌的可行方法,用于增强 IBD 的协同治疗。

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引用本文的文献

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Engineered Probiotic-Based Biomaterials for Inflammatory Bowel Disease Treatment.用于治疗炎症性肠病的工程化益生菌基生物材料
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The therapeutic potential of nanoencapsulated anti-inflammatory drugs delivered to the gut.
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The Gut Microbiota-Xanthurenic Acid-Aromatic Hydrocarbon Receptor Axis Mediates the Anticolitic Effects of Trilobatin.肠道微生物群-黄尿酸-芳香烃受体轴介导三叶苷的抗结肠炎作用。
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