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聚氨酯化学性质和蛋白质涂层对单核细胞向伤口愈合表型巨噬细胞分化的影响。

Effect of polyurethane chemistry and protein coating on monocyte differentiation towards a wound healing phenotype macrophage.

作者信息

McBane Joanne E, Matheson Loren A, Sharifpoor Soroor, Santerre J Paul, Labow Rosalind S

机构信息

Institute of Biomaterials and Biomedical Engineering, University of Toronto, Toronto, ON M5G 1G6, Canada.

出版信息

Biomaterials. 2009 Oct;30(29):5497-504. doi: 10.1016/j.biomaterials.2009.07.010. Epub 2009 Jul 26.

Abstract

Tissue regeneration alternatives for peripheral vascular disease are actively being investigated; however, few studies in this area have probed the role of the wound healing monocyte-derived macrophage (MDM). Inflammatory MDMs transition to wound healing MDMs as the relative levels of tumor necrosis factor-alpha (TNF-alpha) decrease and IL-10 increase. TNF-alpha has been linked to the regulation of HMGB1 (high mobility group box 1 protein), a nuclear protein that upon macrophage stimulation can be secreted and act as a pro-inflammatory cytokine. This study investigated the influence of a degradable polar hydrophobic ionic polyurethane (D-PHI) on MDM cell expression of pro- versus anti-inflammatory markers, when the material was uncoated or pre-coated with collagen prior to cell studies. Effects were compared to similar groups on tissue culture polystyrene (TCPS). Collagen coated TCPS and D-PHI had significantly more DNA than the uncoated TCPS after 7d (p=0.001 and p=0.006 respectively); however, there was significantly less esterase activity from cells on D-PHI (+/-collagen) than for cells on TCPS after 7d (p=0.002, p=0.0003 respectively). No significant differences in esterase activity were observed between collagen coated and non-coated D-PHI surfaces. Analyses of pro-inflammatory cytokines (TNF-alpha, IL-1beta and HMGB1) secreted from differentiating monocytes adherent to D-PHI demonstrated a decrease whereas anti-inflammatory IL-10 increased over time when compared to TCPS, suggesting that D-PHI was less inflammatory than TCPS. Since D-PHI maintains cell attachment while aiding in the transition of MDM to a wound healing phenotype, this material has qualities suitable to be used in tissue engineering applications where MDM play a key role in tissue regeneration.

摘要

外周血管疾病的组织再生替代方案正在积极研究中;然而,该领域很少有研究探讨伤口愈合单核细胞衍生巨噬细胞(MDM)的作用。随着肿瘤坏死因子-α(TNF-α)相对水平降低和白细胞介素-10增加,炎性MDM会转变为伤口愈合MDM。TNF-α与高迁移率族蛋白B1(HMGB1)的调节有关,HMGB1是一种核蛋白,在巨噬细胞受到刺激时可分泌并作为促炎细胞因子发挥作用。本研究调查了可降解极性疏水离子聚氨酯(D-PHI)在细胞研究前未涂层或预涂有胶原蛋白时,对MDM细胞促炎与抗炎标志物表达的影响。将结果与组织培养聚苯乙烯(TCPS)上的类似组进行比较。7天后,胶原蛋白包被的TCPS和D-PHI的DNA含量明显高于未包被的TCPS(分别为p = 0.001和p = 0.006);然而,7天后,D-PHI(有无胶原蛋白)上细胞的酯酶活性明显低于TCPS上细胞的酯酶活性(分别为p = 0.002,p = 0.0003)。在胶原蛋白包被和未包被的D-PHI表面之间未观察到酯酶活性的显著差异。与TCPS相比,对附着在D-PHI上的分化单核细胞分泌的促炎细胞因子(TNF-α、白细胞介素-1β和HMGB1)的分析表明,随着时间的推移,其含量减少,而抗炎性白细胞介素-10增加,这表明D-PHI的炎症性低于TCPS。由于D-PHI在维持细胞附着的同时有助于MDM转变为伤口愈合表型,这种材料具有适合用于MDM在组织再生中起关键作用的组织工程应用的特性。

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