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首页> 外文期刊>Biomaterials >Use of collagen sponge incorporating transforming growth factor-beta1 to promote bone repair in skull defects in rabbits.
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Use of collagen sponge incorporating transforming growth factor-beta1 to promote bone repair in skull defects in rabbits.

机译:胶原蛋白海绵与转化生长因子-β1结合使用以促进兔颅骨缺损的骨修复。

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The objective of this study was to evaluate the potential of collagen sponge incorporating transforming growth factor-beta1 (TGF-beta1) to enhance bone repair. The collagen sponge was prepared by freeze-drying aqueous foamed collagen solution. Thermal cross-linking was performed in a vacuum at 140 degrees C for periods ranging from 1 to 48 h to prepare a number of fine collagen sponges. When collagen sponges incorporating 125I-labeled TGF-beta1 were placed in phosphate-buffered saline (PBS) solution at 37 degrees C, a small amount of TGF-beta1 was released for the first hour, but no further release was observed thereafter, irrespective of the amount of cross-linking time the sponges had received. Collagen sponges incorporating 125I-labeled TGF-beta1 or simply labeled with 125I were implanted into the skin on the backs of mice. The radioactivity of the 125I-labeled TGF-beta1 in the collagen sponges decreased with time; the amount of TGF-beta1 remaining dependent on the cross-linking time. The in vivo retention of TGF-beta1 was longer in those sponges that had been subjected to longer cross-linking times. The in vivo release profile of the TGF-beta1 was matched with the degradation profile of the sponges. Scanning electron microscopic observation revealed no difference in structure among sponges subjected to different cross-linking times. The TGF-beta1 immobilized in the sponges was probably released in vivo as a result of sponge biodegradation because TGF-beta1 release did not occur in in vitro conditions in which sponges did not degrade. We applied collagen sponges incorporating 0.1 microg of TGF-beta1 to skull defects in rabbits in stress-unloaded bone situations. Six weeks later, the skull defects were covered by newly formed bone, in marked contrast to the results obtained with a TGF-beta1 free empty collagen sponge and 0.1 microg of free TGF-beta1. We concluded that the collagen sponges were able to release biologically active TGF-beta1 and were a promising material for bone repair.
机译:这项研究的目的是评估胶原蛋白海绵结合转化生长因子-β1(TGF-β1)增强骨修复的潜力。胶原海绵是通过将泡沫胶原水溶液冷冻干燥而制得的。在真空中在140摄氏度下进行热交联1到48小时,以制备许多细的胶原海绵。将掺有125 I标记的TGF-β1的胶原海绵在37℃的磷酸盐缓冲液(PBS)溶液中放置时,第一小时释放了少量TGF-β1,但此后未观察到进一步释放,无论海绵已经收到的交联时间。将掺有125I标记的TGF-beta1或简单地用125I标记的胶原海绵植入小鼠背部的皮肤中。胶原海绵中125 I标记的TGF-β1的放射性随时间降低;剩余的TGF-beta1量取决于交联时间。在经历了较长交联时间的海绵中,TGF-beta1在体内的保留时间更长。 TGF-β1的体内释放曲线与海绵的降解曲线相匹配。扫描电子显微镜观察表明,在经历不同交联时间的海绵之间的结构没有差异。由于海绵的生物降解作用,固定在海绵中的TGF-β1可能在体内释放,因为在海绵不降解的体外条件下,TGF-β1的释放并未发生。我们在无应力骨骼的情况下,将掺有0.1微克TGF-beta1的胶原蛋白海绵应用于兔子的颅骨缺损。六周后,颅骨缺损被新形成的骨头覆盖,这与使用不含TGF-β1的空胶原海绵和0.1微克游离TGF-β1的结果形成鲜明对比。我们得出的结论是,胶原蛋白海绵能够释放具有生物活性的TGF-beta1,并且是用于骨修复的有前途的材料。

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