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A Review of the Foreign-body Response to Subcutaneously-implanted Devices: The Role of Macrophages and Cytokines in Biofouling and Fibrosis

机译:异物对皮下植入设备的反应的审查:巨噬细胞和细胞因子在生物污染和纤维化中的作用。

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摘要

The biological response to implanted biomaterials in mammals is a complex series of events that involves many biochemical pathways. Shortly after implantation, fibrinogen and other proteins bind to the device surface, a process known as biofouling. Macrophages then bind to receptors on the proteins, join into multinucleated giant cells, and release transforming growth factor β and other inflammatory cytokines. In response to these signals, quiescent fibroblasts are transformed into myofibroblasts, which synthesize procollagen via activation of Smad mediators. The procollagen becomes crosslinked after secretion into the extracellular space. Mature crosslinked collagen and other extracellular matrix proteins gradually contribute to formation of a hypocellular dense fibrous capsule that becomes impermeable or hypopermeable to many compounds. Porous substrates and angiogenic growth factors can stimulate formation of microvessels, which to some extent can maintain analyte delivery to implanted sensors. However, stimulation by vascular endothelial growth factor alone may lead to formation of leaky, thin-walled, immature vessels. Other growth factors are most probably needed to act upon these immature structures to create more robust vessels.
机译:对哺乳动物中植入的生物材料的生物反应是一系列复杂的事件,涉及许多生化途径。植入后不久,纤维蛋白原和其他蛋白质结合到装置表面,这一过程称为生物污染。巨噬细胞然后与蛋白质上的受体结合,加入多核巨细胞,并释放出转化生长因子β和其他炎性细胞因子。响应这些信号,静止的成纤维细胞被转化为成肌纤维细胞,后者通过激活Smad介体来合成胶原蛋白。原胶原在分泌到细胞外空间后变得交联。成熟的交联胶原蛋白和其他细胞外基质蛋白逐渐有助于形成细胞下层致密的纤维囊,该囊对许多化合物变得不可渗透或不可渗透。多孔底物和血管生成生长因子可以刺激微血管的形成,在一定程度上可以维持分析物向植入传感器的传递。然而,仅通过血管内皮生长因子的刺激可能导致形成渗漏的薄壁未成熟血管。其他生长因子最可能需要作用于这些未成熟的结构,以产生更坚固的血管。

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  • 作者

    Kenneth Ward, W.;

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  • 年度 2008
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  • 原文格式 PDF
  • 正文语种 en
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