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Collagen/gold nanoparticle nanocomposites: A potential skin wound healing biomaterial

机译:胶原蛋白/金纳米颗粒纳米复合材料:潜在的皮​​肤伤口愈合生物材料

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In this study, nanocomposite collagen scaffolds incorporating gold nanoparticles (AuNPs) were prepared for wound healing applications. Initially, dose (<20ppm) and size (>20nm) of AuNPs that were not cytotoxic on HaCat keratinocytes and 3T3 fibroblasts were determined. Both collagen sponges and AuNP-incorporated nanocomposites (CS-Au) were cross-linked with glutaraldehyde (CS-X and CS-AuX). Incorporation of AuNPs into cross-linked scaffolds enhanced their stability against enzymatic degradation and increased the tensile strength. Hydrolytic degradation of CS-Au group was also less than CS after seven days. Upon confirming in vitro biocompatibility of the scaffolds with cytotoxicity assays, cell attachment and proliferation tests and the in vivo efficacy for healing of full-thickness skin wounds were investigated by applying CS-X, CS-AuX or a commercial product (Matriderm (R)) onto defect sites and covering with Ioban (R) drapes. Defects were covered only with drapes for untreated control group. The wound areas were examined with histopathological and biomechanical tests after 14 days of operation. CS-AuX group was superior to untreated control and Matriderm (R); it suppressed the inflammation while significantly promoting granulation tissue formation. Inflammatory reaction against CS-AuX was milder than CS-X. Neovascularization was also higher in CS-AuX than other groups, though the result was not significant. Wound closure in CS-X (76%), CS-AuX (69%), and Matriderm (R) (65%) were better than untreated control (45%). CS-AuX group had the highest tensile strength (significantly higher than Matriderm (R)) and modulus (significantly higher than Matriderm (R) and CS-X), indicating a faster course of dermal healing. Further studies are also needed to investigate whether higher loading of AuNPs affects these results positively in a statistically meaningful manner. Overall, their contribution to the enhancement of degradation profiles and mechanical properties, their excellent invitro biocompatibility, and tendency to accelerate wound healing are encouraging the use of AuNPs in collagen sponges as potent skin substitutes in the future.
机译:在这项研究中,制备了掺有金纳米颗粒(AuNPs)的纳米复合胶原蛋白支架,用于伤口愈合应用。最初,确定对HaCat角质形成细胞和3T3成纤维细胞无细胞毒性的AuNP的剂量(<20ppm)和大小(> 20nm)。胶原海绵和掺有AuNP的纳米复合材料(CS-Au)均与戊二醛(CS-X和CS-AuX)交联。将AuNP掺入交联的支架中增强了其抗酶促降解的稳定性并提高了抗张强度。 7天后,CS-Au基团的水解降解也小于CS。通过细胞毒性测定确认支架的体外生物相容性后,通过使用CS-X,CS-AuX或市售产品(Matriderm(R) )到缺陷部位并用Ioban(R)悬垂布覆盖。对于未治疗的对照组,仅用窗帘覆盖缺陷。手术14天后,通过组织病理学和生物力学测试检查伤口区域。 CS-AuX组优于未治疗的对照组和Matriderm(R);它抑制炎症,同时显着促进肉芽组织的形成。针对CS-AuX的炎症反应比CS-X轻。 CS-AuX组的新生血管形成也高于其他组,尽管结果并不明显。 CS-X(76%),CS-AuX(69%)和Matriderm(R)(65%)的伤口闭合效果优于未处理的对照组(45%)。 CS-AuX组的抗张强度最高(显着高于Matridrm(R))和模量(显着高于Matriderm(R)和CS-X),表明皮肤愈合的过程更快。还需要进一步的研究,以研究较高的AuNP含量是否以统计学上有意义的方式对这些结果产生积极影响。总体而言,它们对增强降解曲线和机械性能的贡献,出色的体外生物相容性以及促进伤口愈合的趋势,都鼓励将来在胶原蛋白海绵中使用AuNP作为有力的皮肤替代品。

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