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首页> 外文期刊>Acta biomaterialia >Macrophage-mediated degradation of crosslinked collagen scaffolds.
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Macrophage-mediated degradation of crosslinked collagen scaffolds.

机译:巨噬细胞介导的交联胶原蛋白支架降解。

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Biological scaffolds used in tissue engineering are incorporated in vivo by a process of cellular in-growth, followed by host-mediated degradation and replacement of these scaffolds, in which phagocytic cells from the monocyte/macrophage cell lineage play a key role. The chemical degradation of scaffolds with collagenases is well established, but to date this has not been correlated with an in vitro model of cell mediated scaffold degradation. RAW264.7, a murine monocyte/macrophage cell line, was cultured on collagen scaffolds crosslinked either by dehydrothermal treatment (DHT) or by carbodiimide (EDC). These cells attached to collagen scaffolds, proliferated and exhibited macrophage aggregation to form giant cells. Crosslinking the scaffolds by either DHT or EDC increased the resistance of the scaffold to degradation by macrophages. Increasing the amount of crosslinking in the scaffold made them more resistant to degradation by collagenase. However, while EDC increased the scaffolds' thermal and mechanical properties and decreased the swelling ratio, DHT increased the mechanical properties, but decreased the denaturation temperature and swelling ratio. Altering the scaffold properties by crosslinking affects the rate of degradation by macrophages, and this is correlated with chemical degradation (r=0.658, p<0.01). This will help in the design of scaffolds with task-specific profiles for use in tissue engineering.
机译:组织工程中使用的生物支架通过细胞向内生长的过程被整合到体内,随后宿主介导的降解和替换这些支架,其中单核细胞/巨噬细胞谱系的吞噬细胞起关键作用。用胶原酶对支架进行化学降解已得到充分证实,但是迄今为止,这与细胞介导的支架降解的体外模型尚未相关。将RAW264.7(一种鼠单核/巨噬细胞系)培养在通过脱水热处理(DHT)或碳二亚胺(EDC)交联的胶原蛋白支架上。这些细胞附着在胶原蛋白支架上,增殖并表现出巨噬细胞聚集以形成巨细胞。通过DHT或EDC使支架交联增加了支架对巨噬细胞降解的抵抗力。支架中交联量的增加使它们更耐胶原酶降解。然而,尽管EDC增加了支架的热和机械性能并降低了溶胀率,但DHT增加了机械性能,但降低了变性温度和溶胀率。通过交联改变支架性质会影响巨噬细胞的降解速率,这与化学降解相关(r = 0.658,p <0.01)。这将有助于设计具有特定任务配置文件的支架,用于组织工程。

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