Hepcidin Induces M1 Macrophage Polarization in Monocytes or THP-1 Derived Macrophages

铁调素诱导单核细胞或 THP-1 衍生巨噬细胞中的 M1 巨噬细胞极化

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作者:Enna Liu, Zheng Li, Yan Zhang, Kuisheng Chen

Background

Macrophage polarization plays a critical role in determining the inflammatory states. Hepcidin is a key negative regulator of iron homeostasis and functions. Although hepcidin has been shown to affect ferroportin expression in macrophages, whether it affects macrophage polarization is still largely unknown.

Conclusion

Hepcidin is able to induce macrophage polarization towards M1 type, and might be utilized as a potential M1 macrophage agonist in clinical practice.

Methods

The expression of iNOS and CD206, and the ratio of IFN-γ vs IL-4 in THP-1 derived macrophages upon hepcidin stimulation were evaluated. Further detected was the percentage of CD16+ M1, CD23+ M1, CD10+ M2 and CCL22+ M2 cells in monocyte derived macrophages.

Objective

To address whether hepcidin induces macrophage polarization.

Results

M1 associated molecules were increased in hepcidin-treated cells, yet M2 associated molecules were increased when hepcidin was neutralized. Concomitantly, we observed a significant increase in IRF3 phosphorylation in hepcidin-stimulated cells. However, STAT6 phosphorylation with hepcidin was neutralized.

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