Zdolsek Johann, Eaton John W, Tang Liping
Department of Hand and Plastic Surgery, University Hospital, SE-581 85 Linköping, Sweden.
J Transl Med. 2007 Jul 1;5:31. doi: 10.1186/1479-5876-5-31.
Medical implants often fail as a result of so-called foreign body reactions during which inflammatory cells are recruited to implant surfaces. Despite the clinical importance of this phenomenon, the mechanisms involved in these reactions to biomedical implants in humans are not well understood. The results from animal studies suggest that both fibrinogen adsorption to the implant surface and histamine release by local mast cells are involved in biomaterial-mediated acute inflammatory responses. The purpose of this study was to test this hypothesis in humans.
Thirteen male medical student volunteers (Caucasian, 21-30 years of age) were employed for this study. To assess the importance of fibrinogen adsorption, six volunteers were implanted with polyethylene teraphthalate disks pre-coated with their own (fibrinogen-containing) plasma or (fibrinogen-free) serum. To evaluate the importance of histamine, seven volunteers were implanted with uncoated disks with or without prior oral administration of histamine receptor antagonists. The acute inflammatory response was estimated 24 hours later by measuring the activities of implant-associated phagocyte-specific enzymes.
Plasma coated implants accumulated significantly more phagocytes than did serum coated implants and the recruited cells were predominantly macrophage/monocytes. Administration of both H1 and H2 histamine receptor antagonists greatly reduced the recruitment of macrophages/monocytes and neutrophils on implant surfaces.
In humans--as in rodents--biomaterial-mediated inflammatory responses involve at least two crucial events: histamine-mediated phagocyte recruitment and phagocyte accumulation on implant surfaces engendered by spontaneously adsorbed host fibrinogen. Based on these results, we conclude that reducing fibrinogen:surface interactions should enhance biocompatibility and that administration of histamine receptor antagonists prior to, and shortly after, medical device implantation should improve the functionality and longevity of medical implants.
医疗植入物常常因所谓的异物反应而失效,在此过程中炎症细胞会被募集到植入物表面。尽管这一现象具有临床重要性,但人类对生物医学植入物产生这些反应的机制尚未完全了解。动物研究结果表明,纤维蛋白原吸附到植入物表面以及局部肥大细胞释放组胺均参与生物材料介导的急性炎症反应。本研究的目的是在人类中验证这一假设。
本研究招募了13名男性医学生志愿者(白种人,年龄21 - 30岁)。为评估纤维蛋白原吸附的重要性,6名志愿者植入预先涂有自身(含纤维蛋白原)血浆或(不含纤维蛋白原)血清的聚对苯二甲酸乙二酯圆盘。为评估组胺的重要性,7名志愿者植入未涂层圆盘,部分在植入前口服组胺受体拮抗剂。24小时后通过测量植入物相关吞噬细胞特异性酶的活性来评估急性炎症反应。
血浆涂层植入物比血清涂层植入物积累了显著更多的吞噬细胞,且募集的细胞主要是巨噬细胞/单核细胞。同时给予H1和H2组胺受体拮抗剂可大大减少植入物表面巨噬细胞/单核细胞和中性粒细胞的募集。
在人类中——与啮齿动物一样——生物材料介导的炎症反应至少涉及两个关键事件:组胺介导的吞噬细胞募集以及宿主纤维蛋白原自发吸附导致的吞噬细胞在植入物表面的积累。基于这些结果,我们得出结论,减少纤维蛋白原与表面的相互作用应可增强生物相容性,并且在医疗器械植入前及植入后不久给予组胺受体拮抗剂应可改善医疗植入物的功能和使用寿命。
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