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肝素化纤维蛋白与胶原海绵作为骨形态发生蛋白-2载体在骨再生中的比较。

Comparison between heparin-conjugated fibrin and collagen sponge as bone morphogenetic protein-2 carriers for bone regeneration.

机构信息

School of Chemical and Biological Engineering, Seoul National University, Seoul 151-744, Korea Bio-Max Institute, Institute of Chemical Process, Engineering Research Institute, Seoul National University, Seoul 151-744, Korea.

出版信息

Exp Mol Med. 2012 May 31;44(5):350-5. doi: 10.3858/emm.2012.44.5.039.

Abstract

Bone morphogenetic protein-2 (BMP-2) is used to promote bone regeneration. However, the bone regeneration ability of BMP-2 relies heavily on the delivery vehicle. Previously, we have developed heparin- conjugated fibrin (HCF), a vehicle for long-term delivery of BMP-2 and demonstrated that long-term delivery of BMP-2 enhanced its osteogenic efficacy as compared to short-term delivery at an equivalent dose. The aim of this study was to compare the bone-forming ability of the BMP-2 delivered by HCF to that delivered by clinically utilized BMP-2 delivery vehicle collagen sponge. An in vitro release profile of BMP-2 showed that HCF released 80% of the loaded BMP-2 within 20 days, whereas collagen sponge released the same amount within the first 6 days. Moreover, the BMP-2 released from the HCF showed significantly higher alkaline phosphatase activity than the BMP-2 released from collagen sponge at 2 weeks in vitro. Various doses of BMP-2 were delivered with HCF or collagen sponge to mouse calvarial defects. Eight weeks after the treatment, bone regeneration was evaluated by computed tomography, histology, and histomorphometric analysis. The dose of BMP-2 delivered by HCF to achieve 100% bone formation in the defects was less than half of the BMP-2 dose delivered by collagen sponge to achieve a similar level of bone formation. Additionally, bone regenerated by the HCF-BMP-2 had higher bone density than bone regenerated by the collagen sponge-BMP-2. These data demonstrate that HCF as a BMP-2 delivery vehicle exerts better osteogenic ability of BMP-2 than collagen sponge, a clinically utilized delivery vehicle.

摘要

骨形态发生蛋白-2(BMP-2)用于促进骨再生。然而,BMP-2 的骨再生能力严重依赖于输送载体。以前,我们开发了肝素结合纤维蛋白(HCF),这是一种长期输送 BMP-2 的载体,并证明与等量的短期输送相比,长期输送 BMP-2 增强了其成骨功效。本研究旨在比较 HCF 输送的 BMP-2 与临床应用的 BMP-2 输送载体胶原海绵的成骨能力。BMP-2 的体外释放曲线表明,HCF 在 20 天内释放了 80%的加载 BMP-2,而胶原海绵在最初 6 天内释放了相同量的 BMP-2。此外,HCF 释放的 BMP-2 在体外 2 周时显示出比胶原海绵释放的 BMP-2 更高的碱性磷酸酶活性。将各种剂量的 BMP-2 用 HCF 或胶原海绵输送到小鼠颅骨缺损处。治疗 8 周后,通过计算机断层扫描、组织学和组织形态计量学分析评估骨再生情况。HCF 输送的 BMP-2 达到 100%骨形成的剂量小于胶原海绵输送的 BMP-2 达到相似骨形成水平的剂量的一半。此外,HCF-BMP-2 再生的骨比胶原海绵-BMP-2 再生的骨具有更高的骨密度。这些数据表明,作为 BMP-2 输送载体的 HCF 比临床应用的输送载体胶原海绵具有更好的 BMP-2 成骨能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4842/3366328/5d849cda9e1d/emm-44-350-g001.jpg

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