首页> 外文期刊>Journal of materials science >Osteoinduction and -conduction through absorbable bone substitute materials based on calcium sulfate: in vivo biological behavior in a rabbit model
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Osteoinduction and -conduction through absorbable bone substitute materials based on calcium sulfate: in vivo biological behavior in a rabbit model

机译:通过可吸收的基于硫酸钙的骨替代材料进行骨诱导和传导:在兔模型中的体内生物学行为

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摘要

Calcium sulfate (CS) can be used as an antibiotically impregnated bone substitute in a variety of clinical constellations. Antibiotically loaded bone substitutes find specific application in orthopedic and trauma surgery to prevent or treat bone infections especially in relation to open bone defects. However, its use as a structural bone graft reveals some concerns due to its fast biodegradation. The addition of calcium carbonate and tripalmitin makes CS formulations more resistant to resorption leaving bone time to form during a prolonged degradation process. The aim of the present study was the evaluation of biocompatibility and degradation properties of newly formulated antibiotically impregnated CS preparations. Three different types of CS bone substitute beads were implanted into the tibial metaphysis of rabbits (CS dihydrate with tripalmitin, containing gentamicin (Group A) or vancomycin (Group B); Group C: tobramycin-loaded CS hemihydrate). Examinations were performed by means of x-ray, micro-computed tomography (micro-CT) and histology after 4, 6, 8 and 12 weeks. Regarding biocompatibility of the formulations, no adverse reactions were observed. Histology showed formation of vital bone cells attached directly to the implanted materials, while no cytotoxic effect in the surrounding of the beads was detected. All CS preparations showed osteogenesis associated to implanted material. Osteoblasts attached directly to the implant surface and revealed osteoid production, osteocytes were found in newly mineralized bone. Group C implants (Osteoset (R)) were subject to quick degradation within 4 weeks, after 6-8 weeks there were only minor remnants with little osteogenesis demonstrated by histological investigations. Group A implants (Herafill (R) - G) revealed similar degradation within atleast 12 weeks. In contrast, group B implants (CaSO4-V) were still detectable after 12 weeks with the presence of implant-associated osteogenesis atlatest follow-up. In all of these preparations, giant cells were found during implant degradation on surface and inside of resorption lacunae. None of the analyzed CS preparations triggered contact activation. All implants demonstrated excellent biocompatibility, with implants of Group A and B showing excellent features as osteo-conductive and -inductive scaffolds able to improve mechanical stability.
机译:硫酸钙(CS)可以用作多种临床星座中的抗生素浸渍骨替代品。载有抗生素的骨替代物在骨科和创伤外科手术中具有特定的应用,可预防或治疗骨感染,尤其是与开放性骨缺损有关的骨感染。然而,由于其快速的生物降解作用,其用作结构性骨移植物引起了一些关注。碳酸钙和三棕榈精的添加使CS配方对吸收的抵抗力增强,从而在长时间的降解过程中形成了骨骼。本研究的目的是评估新配制的抗生素浸渍CS制剂的生物相容性和降解特性。将三种不同类型的CS骨替代珠植入兔的胫骨干physi端(CS与三苯甲酰胺二水合物,含有庆大霉素(A组)或万古霉素(B组); C组:载有妥布霉素的CS半水合物)。在4、6、8和12周后,通过X射线,微型计算机断层扫描(micro-CT)和组织学进行检查。关于制剂的生物相容性,未观察到不良反应。组织学显示直接连接到植入材料上的重要骨细胞形成,而在珠子周围未检测到细胞毒性作用。所有CS制剂均显示出与植入材料相关的成骨作用。成骨细胞直接附着在植入物表面并显示出类骨质产生,在新矿化的骨中发现了骨细胞。 C组植入物(Osteoset(R))在4周内迅速降解,在6-8周后,仅有少量残余物,组织学研究显示几乎没有成骨作用。 A组植入物(Herafill(R)-G)在至少12周内显示出类似的降解。相反,B组植入物(CaSO4-V)在12周后仍可检出,并且在后续随访中存在植入物相关的成骨作用。在所有这些制剂中,在吸收腔的表面和内部的植入物降解过程中都发现了巨细胞。分析的CS准备均未触发接触激活。所有植入物均表现出优异的生物相容性,而A组和B组的植入物表现出优异的功能,如骨传导性和诱导性支架能够改善机械稳定性。

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  • 来源
    《Journal of materials science》 |2018年第2期|17.1-17.14|共14页
  • 作者单位

    Tech Univ Munich, Klinikum Rechts Isar, Klin & Poliklin Unfallchirurg, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin & Poliklin Unfallchirurg, Munich, Germany;

    Chirurg Klinikum Munchen Sud, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

    Tech Univ Munich, Klinikum Rechts Isar, Klin Orthopadie & Sportorthopadie, Munich, Germany;

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