Mechanical Strength, Biodegradation, and in Vitro and in Vivo Biocompatibility of Zn Biomaterials

生物相容性 材料科学 体内 生物医学工程 腐蚀 组织工程 模拟体液 溶血 活力测定 极限抗拉强度 体外 冶金 复合材料 化学 医学 生物化学 扫描电子显微镜 免疫学 生物技术 生物
作者
Donghui Zhu,Irsalan Cockerill,Yingchao Su,Zhaoxiang Zhang,Jiayin Fu,Kee-Won Lee,Jun Ma,Chuka Okpokwasili,Liping Tang,Yufeng Zheng,Yi‐Xian Qin,Yadong Wang
出处
期刊:ACS Applied Materials & Interfaces [American Chemical Society]
卷期号:11 (7): 6809-6819 被引量:143
标识
DOI:10.1021/acsami.8b20634
摘要

Zn-based biomaterials have emerged as promising new types of bioresorbable metallics applicable to orthopedic devices, cardiovascular stents, and other medical applications recently. Compared to other degradable metallic biomaterials (i.e., Mg- or Fe-based), Zn biomaterials have a more appropriate corrosion rate without hydrogen gas evolution. Here, we evaluated the potential of Zn-based metallics as medical implants, both in vitro and in vivo, alongside a standard benchmark Mg alloy, AZ31. The mechanical properties of the pure Zn were not strong enough but were significantly enhanced (microhardness > 70 kg/mm2, strength > 220 MPa, elongation > 15%) after alloying with Sr or Mg (1.5 at. %), surpassing the minimal design criteria for load-bearing device applications. The corrosion rate of Zn-based biomaterials was about 0.4 mm/year, significantly slower than that of AZ31. The measured cell viability and proliferation of three different human primary cells fared better for Zn-based biomaterials than AZ31 using both direct and indirect culture methods. Platelet adhesion and activation on Zn-based materials were minimal, significantly less than on AZ31. The hemolysis ratio of red cells (<0.5%) after incubation with Zn-based materials was also well below the ISO standard of 5%. Moreover, Zn-based biomaterials promoted stem cell differentiation to induce the extracellular matrix mineralization process. In addition, in vivo animal testing using subcutaneous, bone, and vascular implantations revealed that the acute toxicity and immune response of Zn-based biomaterials were minimal/moderate, comparable to that of AZ31. No extensive cell death and foreign body reactions were observed. Taken together, Zn-based biomaterials may have a great potential as promising candidates for medical implants.
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