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Matrix crosslinking enhances macrophage adhesion migration and inflammatory activation

机译:基质交联可增强巨噬细胞的粘附迁移和炎症激活

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摘要

Macrophages are versatile cells of the innate immune system that can adopt a variety of functional phenotypes depending on signals in their environment. In previous work, we found that culture of macrophages on fibrin, the provisional extracellular matrix protein, inhibits their inflammatory activation when compared to cells cultured on polystyrene surfaces. Here, we sought to investigate the role of matrix stiffness in the regulation of macrophage activity by manipulating the mechanical properties of fibrin. We utilize a photo-initiated crosslinking method to introduce dityrosine crosslinks to a fibrin gel and confirm an increase in gel stiffness through active microrheology. We observe that matrix crosslinking elicits distinct changes in macrophage morphology, integrin expression, migration, and inflammatory activation. Macrophages cultured on a stiffer substrate exhibit greater cell spreading and expression of αM integrin. Furthermore, macrophages cultured on crosslinked fibrin exhibit increased motility. Finally, culture of macrophages on photo-crosslinked fibrin enhances their inflammatory activation compared to unmodified fibrin, suggesting that matrix crosslinking regulates the functional activation of macrophages. These findings provide insight into how the physical properties of the extracellular matrix might control macrophage behavior during inflammation and wound healing.
机译:巨噬细胞是先天免疫系统的通用细胞,根据其环境中的信号,它们可以采用多种功能表型。在以前的工作中,我们发现与在聚苯乙烯表面培养的细胞相比,在纤维蛋白(临时的细胞外基质蛋白)上培养巨噬细胞可抑制其炎症激活。在这里,我们试图通过操纵纤维蛋白的机械性能来研究基质刚度在巨噬细胞活性调节中的作用。我们利用光引发的交联方法将二酪氨酸交联引入纤维蛋白凝胶,并通过活性微流变学确定凝胶刚度的增加。我们观察到基质交联引起巨噬细胞形态,整联蛋白表达,迁移和炎症激活的明显变化。培养在较硬底物上的巨噬细胞表现出更大的细胞扩散和αM整联蛋白表达。此外,在交联的纤维蛋白上培养的巨噬细胞显示出增加的运动性。最后,与未修饰的血纤蛋白相比,在光交联的血纤蛋白上培养巨噬细胞可增强其炎症激活,表明基质交联调节巨噬细胞的功能激活。这些发现提供了洞察细胞外基质的物理特性在炎症和伤口愈合过程中如何控制巨噬细胞行为的见解。

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