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铜离子和镁离子与低浓度地塞米松联用对巨噬细胞反应的调节作用

Modulation of Macrophage Response by Copper and Magnesium Ions in Combination with Low Concentrations of Dexamethasone.

作者信息

Díez-Tercero Leire, Delgado Luis M, Perez Roman A

机构信息

Bioengineering Institute of Technology, Universitat Internacional de Catalunya, Sant Cugat del Vallès, 08195 Barcelona, Spain.

Basic Science Department, Universitat Internacional de Catalunya, Sant Cugat del Vallès, 08195 Barcelona, Spain.

出版信息

Biomedicines. 2022 Mar 24;10(4):764. doi: 10.3390/biomedicines10040764.

Abstract

Macrophages have been deemed crucial for correct tissue regeneration, which is a complex process with multiple overlapping phases, including inflammation. Previous studies have suggested that divalent ions are promising cues that can induce an anti-inflammatory response, since they are stable cues that can be released from biomaterials. However, their immunomodulatory potential is limited in a pro-inflammatory environment. Therefore, we investigated whether copper and magnesium ions combined with low concentrations of the anti-inflammatory drug, dexamethasone (dex), could have a synergistic effect in macrophage, with or without pro-inflammatory stimulus, in terms of morphology, metabolic activity and gene expression. Our results showed that the combination of copper and dex strongly decreased the expression of pro-inflammatory markers, while the combination with magnesium upregulated the expression of IL-10. Moreover, in the presence of a pro-inflammatory stimulus, the combination of copper and dex induced a strong TNF-α response, suggesting an impairment of the anti-inflammatory actions of dex. The combination of magnesium and dex in the presence of a pro-inflammatory stimulus did not promote any improvement in comparison to dex alone. The results obtained in this study could be relevant for tissue engineering applications and in the design of platforms with a dual release of divalent ions and small molecules.

摘要

巨噬细胞被认为对正确的组织再生至关重要,组织再生是一个复杂的过程,有多个重叠阶段,包括炎症阶段。先前的研究表明,二价离子是有前景的信号,可诱导抗炎反应,因为它们是可从生物材料中释放的稳定信号。然而,在促炎环境中,它们的免疫调节潜力有限。因此,我们研究了铜离子和镁离子与低浓度抗炎药物地塞米松(dex)联合使用,在有无促炎刺激的情况下,对巨噬细胞的形态、代谢活性和基因表达是否具有协同作用。我们的结果表明,铜离子和地塞米松联合使用可强烈降低促炎标志物的表达,而与镁离子联合使用则上调白细胞介素-10的表达。此外,在存在促炎刺激的情况下,铜离子和地塞米松联合使用会诱导强烈的肿瘤坏死因子-α反应,这表明地塞米松的抗炎作用受到损害。与单独使用地塞米松相比,在存在促炎刺激的情况下,镁离子和地塞米松联合使用并没有带来任何改善。本研究获得的结果可能与组织工程应用以及设计具有二价离子和小分子双重释放功能的平台相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2030/9030383/e2f30095b524/biomedicines-10-00764-g001.jpg

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