Exosomes from mesenchymal stromal cells reduce murine colonic inflammation via a macrophage-dependent mechanism
Huashan Liu, Zhenxing Liang, Fengwei Wang, Chi Zhou, Xiaobin Zheng, Tuo Hu, Xiaowen He, Xianrui Wu, Ping Lan
Huashan Liu, Zhenxing Liang, Fengwei Wang, Chi Zhou, Xiaobin Zheng, Tuo Hu, Xiaowen He, Xianrui Wu, Ping Lan
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Research Article Stem cells Therapeutics

Exosomes from mesenchymal stromal cells reduce murine colonic inflammation via a macrophage-dependent mechanism

Abstract

Conventional treatments for inflammatory bowel disease (IBD) have multiple potential side effects. Therefore, alternative treatments are desperately needed. This work demonstrated that systemic administration of exosomes from human bone marrow–derived mesenchymal stromal cells (MSC-Exos) substantially mitigated colitis in various models of IBD. MSC-Exos treatment downregulated inflammatory responses, maintained intestinal barrier integrity, and polarized M2b macrophages but did not favor intestinal fibrosis. Mechanistically, infused MSC-Exos acted mainly on colonic macrophages, and macrophages from colitic colons acquired obvious resistance to inflammatory restimulation when prepared from mice treated with MSC-Exos versus untreated mice. The beneficial effect of MSC-Exos was blocked by macrophage depletion. Also, the induction of IL-10 production from macrophages was partially involved in the beneficial effect of MSC-Exos. MSC-Exos were enriched in proteins involved in regulating multiple biological processes associated with the anticolitic benefit of MSC-Exos. Particularly, metallothionein-2 in MSC-Exos was required for the suppression of inflammatory responses. Taken together, MSC-Exos are critical regulators of inflammatory responses and may be promising candidates for IBD treatment.

Authors

Huashan Liu, Zhenxing Liang, Fengwei Wang, Chi Zhou, Xiaobin Zheng, Tuo Hu, Xiaowen He, Xianrui Wu, Ping Lan

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Figure 3

Anticolitic benefit of MSC-Exos in DSS-induced chronic and recurrent colitis.

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Anticolitic benefit of MSC-Exos in DSS-induced chronic and recurrent col...
Male C57BL/6 mice at 6–8 weeks of age (n = 20 mice per group) were subjected to 3% DSS in the drinking water in a cyclic manner. Each cycle consisted of 7 days of DSS followed by a 7-day phase without DSS supplementation. MSC-Exos (200 μg/mouse) were infused intravenously on day 7 or on days 7 and 16 (arrows in A). DAI (A) and mortality (B) were recorded. (C) Measurements of colon lengths. (D) Histopathological changes. Original magnification, ×100 (left), ×200 (right). (E) Semiquantitative scoring of histopathology. (F) Neutrophil infiltration determined by measuring colonic MPO activity on day 28. The number of animals studied is shown in each figure. *P ≤ 0.05, **P ≤ 0.01, and ***P ≤ 0.001, by Kruskal-Wallis test (A, E, and F), log-rank test (B), or 1-way ANOVA (C).