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Strontium and magnesium ions released from bioactive titanium metal promote early bone bonding in a rabbit implant model

机译:从生物活性钛金属释放的锶和镁离子促进兔植入模型中的早期骨键合

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摘要

Graphical abstract Display Omitted Abstract We have previously developed the “alkali and heat treatment” method to confer bioactivity (bone-bonding ability) to titanium metal (Ti). As strontium (Sr) and magnesium (Mg) ions reportedly promote osteoblastic cell proliferation and differentiation and accelerate bone formation, we improved this method to induce the release of Sr (Sr-Ti) or Mg (Mg-Ti) ions from Ti in a previous study. Here, we evaluated the bioactivity of these novel surface treatments, Sr-Ti and Mg-Ti. In vitro evaluation of cell viability, expression of integrin β1 , β catenin , and cyclin D1 , osteogenic gene expression, alkaline phosphatase activity, and extracellular mineralization using MC3T3-E1 cells revealed that Sr-Ti and Mg-Ti enhanced proliferation and osteogenic differentiation. In rabbit in vivo studies, Sr-Ti and Mg-Ti also provided greater biomechanical strength and bone-implant contact than the positive control Ti (Ca-Ti), especially at the early stage (4–8weeks), and maintained these properties for a longer period (16–24weeks). Advantages of the improved method include process simplicity, applicability for any implant shape, and lack of adverse effects on implant composition and structure. Therefore, our treatment is promising for clinical applications to achieve early bone bonding. Statement of Significance Implantation into osteoporotic bone constitutes a challenging problem because of early migration or loosening of the implant, which is primarily due to insufficient initial fixation in porotic bone. Therefore, it is desirable to provide implants with a capacity for early bone bonding. We have achieved conferring early bone bonding ability to titanium metal by releasing strontium ions or magnesium ions. Our treatment is promising for clinical applications to achieve early bone bonding of orthopedic or dental Ti-based implants.
机译:图形摘要显示省略摘要我们以前开发了“碱和热处理”方法,以赋予钛金属(Ti)的生物活性(骨粘合能力)。作为锶(Sr)和镁(Mg)离子促进了骨细胞细胞增殖和分化并加速骨形成,我们改进了该方法,以诱导来自Ti中的Sr(Sr-Ti)或Mg(Mg-Ti)离子的释放以前的研究。在这里,我们评估了这些新型表面处理,SR-Ti和Mg-Ti的生物活性。使用MC3T3-E1细胞的细胞活力的体外评估细胞活力,整联β1,β1,β1,βcatenin和Cyclin D1,osteogens基因表达,碱性磷酸酶活性和细胞外矿化,显示SR-Ti和Mg-Ti增强了增殖和骨质发生分化。在体内研究中,SR-Ti和Mg-Ti还提供了更大的生物力学强度和骨植入接触,而不是阳性对照Ti(Ca-Ti),特别是在早期(4-8周),并保持这些性质更长的时间(16-24周)。改进方法的优点包括工艺简单性,适用于任何植入形状,以及对植入物组成和结构的缺乏不利影响。因此,我们的待遇是对临床应用有望实现早期骨键的临床应用。由于早期迁移或松动植入物,植入骨植入意义植入骨质骨骼的陈述构成了一个具有挑战性的问题,这主要是由于姿势骨的初始固定不充分。因此,希望提供具有早期骨粘合能力的植入物。通过释放锶离子或镁离子,我们已经实现了赋予钛金属的早期骨键合能力。我们的治疗是对临床应用的临床应用,以实现整形外科或牙科Ti植入物的早期骨键。

著录项

  • 来源
    《Acta biomaterialia》 |2017年第2017期|共10页
  • 作者单位

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Biomedical Sciences College of Life and Health Sciences Chubu University;

    Department of Biomedical Engineering Faculty of Life and Medical Sciences Doshisha University;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

    Department of Biomedical Sciences College of Life and Health Sciences Chubu University;

    Department of Biomedical Sciences College of Life and Health Sciences Chubu University;

    Department of Orthopaedic Surgery Kyoto University Graduate School of Medicine;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 普通生物学;
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