Milk-derived extracellular vesicles alleviate ulcerative colitis by regulating the gut immunity and reshaping the gut microbiota

Lingjun Tong; Haining Hao; Zhe Zhang; Youyou Lv; Xi Liang; Qiqi Liu; Tongjie Liu; Pimin Gong; Lanwei Zhang; Fangfang Cao; Giorgia Pastorin; Chuen Neng Lee; Xiaoyuan Chen; Jiong‐Wei Wang; Huaxi Yi

doi:10.7150/thno.62046

Milk-derived extracellular vesicles alleviate ulcerative colitis by regulating the gut immunity and reshaping the gut microbiota

Lingjun Tong(National University of Singapore), Haining Hao(Ocean University of China), Zhe Zhang(Ocean University of China), Youyou Lv(Ocean University of China), Xi Liang(Ocean University of China), Qiqi Liu(Ocean University of China), Tongjie Liu(Ocean University of China), Pimin Gong(Ocean University of China), Lanwei Zhang(Ocean University of China), Fangfang Cao(National University of Singapore), Giorgia Pastorin(National University of Singapore), Chuen Neng Lee(National University of Singapore), Xiaoyuan Chen(National University of Singapore), Jiong‐Wei Wang(National University of Singapore), Huaxi Yi(Ministry of Education)

Theranostics

January 1, 2021

10.7150/thno.62046

Cited by 311Open Access

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Abstract

Rationale: Bovine milk constitutes an essential part of human diet, especially for children, due to its enrichment of various nutrients. We recently developed an effective protocol for the isolation of extracellular vesicles from milk (mEVs) and discovered that mEVs contained large amounts of immune-active proteins and modulated the gut immunity and microbiota in healthy mice. Here, we aimed to explore the therapeutic effects of mEVs on inflammatory bowel disease. Methods: MicroRNAs and protein content in mEVs were analyzed by RNA sequencing and proteomics, respectively, followed by functional annotation. Ulcerative colitis (UC) was induced by feeding mice with dextran sulfate sodium. Intestinal immune cell populations were phenotyped by flow cytometry, and the gut microbiota was analyzed via 16S rRNA sequencing. Results: We showed that abundant proteins and microRNAs in mEVs were involved in the regulation of immune and inflammatory pathways and that oral administration of mEVs prevented colon shortening, reduced intestinal epithelium disruption, inhibited infiltration of inflammatory cells and tissue fibrosis in a mouse UC model. Mechanistically, mEVs attenuated inflammatory response via inhibiting TLR4-NF-B signaling pathway and NLRP3 inflammasome activation. Furthermore, mEVs were able to correct cytokine production disorder and restore the balance between T helper type 17 (Th17) cells and interleukin-10 + Foxp3 + regulatory T (Treg) cells in the inflamed colon. The disturbed gut microbiota in UC was also partially recovered upon treatment with mEVs. The correlation between the gut microbiota and cytokines suggests that mEVs may modulate intestinal immunity via influencing the gut microbiota. Conclusions: These findings reveal that mEVs alleviate colitis by regulating intestinal immune homeostasis via inhibiting TLR4-NF-B and NLRP3 signaling pathways, restoring Treg/Th17 cell balance, and reshaping the gut microbiota.

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