首页> 美国卫生研究院文献>Frontiers in Endocrinology >Effects of Vitamin E-Stabilized Ultra High Molecular Weight Polyethylene on Oxidative Stress Response and Osteoimmunological Response in Human Osteoblast
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Effects of Vitamin E-Stabilized Ultra High Molecular Weight Polyethylene on Oxidative Stress Response and Osteoimmunological Response in Human Osteoblast

机译:维生素E稳定的超高分子量聚乙烯对成骨细胞氧化应激反应和骨免疫反应的影响

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摘要

High Crosslink process was introduced in the development of joint prosthetic devices, in order to decrease the wear rate of ultrahigh molecular weight polyethylene (UHMWPE), but it also triggers the formation of free radicals and oxidative stress, which affects the physiological bone remodeling, leading to osteolysis. Vitamin E stabilization of UHMWPE was proposed to provide oxidation resistance without affecting mechanical properties and fatigue strength. The aim of this study is to evaluate the antioxidant effect of vitamin E added to UHMWPE on oxidative stress induced osteolysis, focusing in particular on the oxidative stress response in correlation with the production of osteoimmunological markers, Sclerostin and DKK-1, and the RANKL/OPG ratio compared to conventional UHMWPE wear debris. Human osteoblastic cell line SaOS2 were incubated for 96 h with wear particles derived from crosslinked and not crosslinked Vitamin E-stabilized, UHMWPE without Vitamin E, and growth medium as control. Cellular response to oxidative stress, compared to not treat cells, was evaluated in terms of proteins O-GlcNAcylation, cellular levels of OGA, and OGT proteins by immunoblotting. O-GlcNAcylation and its positive regulator OGT levels are increased in the presence of Vitamin E blended UHMWPE, in particular with not crosslinked Vit E stabilized UHMWPE. Conversely, the negative regulator OGA increased in the presence of UHMWPE not blended with Vitamin E. Vitamin E-stabilized UHMWPE induced a decrease of RANKL/OPG ratio compared to UHMWPE without Vitamin E, and the same effect was observed for Sclerostin, while DKK-1 was not significantly affected. In conclusion, Vitamin E stabilization of UHMWPE increased osteoblast response to oxidative stress, inducing a cellular mechanism aimed at cell survival. Vitamin E antioxidant effect influences the secretion of osteoimmunological factors, shifting the bone turnover balance toward bone protection stimuli. This suggests that Vitamin E-Stabilization of UHMWPE could contribute to reduction of oxidation-induced osteolysis and the consequent loosening of the prosthetic devices, therefore improving the longevity of total joint replacements.
机译:为了减少超高分子量聚乙烯(UHMWPE)的磨损率,在关节修复设备的开发过程中引入了高交联工艺,但它也触发了自由基的形成和氧化应激,从而影响了骨骼的生理重塑,导致去溶骨。提出了UHMWPE的维生素E稳定化以提供抗氧化性,而不影响机械性能和疲劳强度。这项研究的目的是评估添加到UHMWPE中的维生素E对氧化应激诱导的骨溶解的抗氧化作用,尤其是与骨免疫标记物Sclerostin和DKK-1以及RANKL /的产生相关的氧化应激反应。与传统的UHMWPE磨屑相比,OPG比率。将人成骨细胞系SaOS2与衍生自交联且未交联的维生素E稳定的磨损颗粒,不含维生素E的UHMWPE和生长培养基作为对照孵育96小时。与未处理的细胞相比,通过免疫印迹,根据蛋白质O-GlcNAcylation,细胞水平的OGA和OGT蛋白质评估了细胞对氧化应激的反应。在维生素E共混的UHMWPE的存在下,尤其是在未交联的Vit E稳定的UHMWPE的存在下,O-GlcNAcylation及其正调节剂OGT的水平会增加。相反,在未与维生素E混合的UHMWPE存在下,负调节剂OGA升高。与不含维生素E的UHMWPE相比,维生素E稳定的UHMWPE导致RANKL / OPG比例降低,并且硬化蛋白和DKK- 1个没有受到明显影响。总之,UHMWPE的维生素E稳定化增加了成骨细胞对氧化应激的反应,诱导了针对细胞存活的细胞机制。维生素E的抗氧化剂作用会影响骨免疫因子的分泌,使骨骼更新平衡朝着骨骼保护刺激方向发展。这表明UHMWPE的维生素E稳定化可能有助于减少氧化诱导的骨溶解并因此导致假体装置松动,从而提高了全关节置换的寿命。

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