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首页> 外文期刊>Acta biomaterialia >Differentiation of monocytes on a degradable, polar, hydrophobic, ionic polyurethane: Two-dimensional films vs. three-dimensional scaffolds.
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Differentiation of monocytes on a degradable, polar, hydrophobic, ionic polyurethane: Two-dimensional films vs. three-dimensional scaffolds.

机译:在可降解的极性疏水性离子聚氨酯上的单核细胞分化:二维膜与三维支架。

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摘要

A degradable, polar, hydrophobic, ionic polyurethane (D-PHI), with physical properties comparable to those of peripheral arterial vascular tissue, was evaluated for monocyte interactions with two different physical forms: two-dimensional films and three-dimensional porous scaffolds. Monocytes, isolated from human whole blood, were seeded onto D-PHI films and scaffolds, and differentiated to monocyte-derived macrophages (MDM) for up to 28 days. The effect of surface structure on the MDM phenotype was assessed by assaying: cell attachment (DNA), activation (intracellular protein expression, esterase and acid phosphatase (AP) activity) as well as pro- and anti-inflammatory cytokines (TNF-alpha and IL-10, respectively). The cells on scaffolds exhibited an initial peak in total protein synthesized per DNA at 3 days; however, both substrates generated similar protein levels per DNA at all other time points. While scaffolds generated more esterase and AP per cell than for films, the cells on films expressed significantly more of these two proteins relative to their total protein produced. At day 7 (acute phase of monocyte activation), cells on films were significantly more activated than monocytes on the scaffolds as assessed by cell morphology and tumor necrosis factor-alpha and interleukin-10 levels. Histological analysis of scaffolds showed that cells were able to migrate throughout the three-dimensional matrix. By inducing a low inflammatory, high wound-healing phenotype monocyte, the negative effects of the foreign body reaction in vivo may be controlled in a manner possible to direct the vascular tissue cells into the appropriate functional phenotypes necessary for successful tissue engineering.
机译:对可降解的极性疏水性离子型聚氨酯(D-PHI)进行了物理性能与外周动脉血管组织相当的评估,评估了单核细胞与两种不同物理形式的相互作用:二维薄膜和三维多孔支架。从人全血中分离出的单核细胞播种到D-PHI膜和支架上,并分化为单核细胞衍生的巨噬细胞(MDM)长达28天。通过以下方法评估表面结构对MDM表型的影响:细胞附着(DNA),激活(细胞内蛋白表达,酯酶和酸性磷酸酶(AP)活性)以及促炎和消炎细胞因子(TNF-α和IL-10)。支架上的细胞在3天时每个DNA合成的总蛋白质中显示出一个初始峰。但是,在所有其他时间点,两种底物的每个DNA产生的蛋白质水平相似。尽管每个细胞比膜产生更多的酯酶和AP,但相对于产生的总蛋白,膜上的细胞表达的这两种蛋白明显更多。在第7天(单核细胞活化的急性期),通过细胞形态,肿瘤坏死因子-α和白细胞介素10水平评估,膜上的细胞比支架上的单核细胞活化得多。支架的组织学分析表明,细胞能够在整个三维矩阵中迁移。通过诱导低炎症性,高伤口愈合表型单核细胞,可以以可能的方式控制体内组织异物反应的负面影响,以使血管组织细胞成为成功进行组织工程所需的适当功能性表型。

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