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首页> 外文期刊>Journal of neurosurgery. >Bone regeneration at rabbit skull defects treated with transforming growth factor-beta1 incorporated into hydrogels with different levels of biodegradability.
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Bone regeneration at rabbit skull defects treated with transforming growth factor-beta1 incorporated into hydrogels with different levels of biodegradability.

机译:用转化生长因子-β1处理的兔颅骨缺损处的骨再生,并以不同水平的生物降解能力将其掺入水凝胶中。

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OBJECT: Skull bone regeneration induced by transforming growth factor-beta1 (TGFbeta1)-containing gelatin hydrogels (TGFbeta1-hydrogels) was investigated using a rabbit skull defect model. Different strengths of TGFbeta1 were examined and compared: different TGFbeta1 doses in gelatin hydrogels with a fixed water content, different water contents in gelatin hydrogels with a fixed TGFbeta1 dose, and TGFbeta1 in solution form. In addition, regenerated skull bone was observed over long time periods after treatment. METHODS: Soft x-ray, dual energy x-ray absorptometry, and histological studies were performed to assess the time course of bone regeneration at a 6-mm-diameter skull defect in rabbits after treatment with TGFbeta1-hydrogels or other agents. The influence of TGFbeta1 dose and hydrogel water content on skull bone regeneration by TGFbeta1-hydrogels was evaluated. Gelatin hydrogels with a water content of 95 wt% that incorporated at least 0.1 microg of TGFbeta1 induced significant bone regeneration at the rabbit skull defect site 6 weeks after treatment, whereas TGFbeta1 in solution form was ineffective, regardless of dose. The in vivo degradability of the hydrogels, which varied according to water content, played an important role in skull bone regeneration induced by TGFbeta1 -hydrogels. In our hydrogel system, TGFbeta1 is released from hydrogels as a result of hydrogel degradation. When the hydrogel degrades too quickly, it does not retain TGFbeta1 or prevent ingrowth of soft tissues at the skull defect site and does not induce bone regeneration at the skull defect. It is likely that hydrogel that degrades too slowly physically impedes formation of new bone at the skull defect. Following treatment with 0.1-microg TGFbeta1-hydrogel (95 wt%), newly formed bone remained at the defect site without being resorbed 6 and 12 months later. The histological structure of the newly formed bone was similar to that of normal skull bone. Overgrowth of regenerated bone and tissue reaction were not observed after treatment with TGFbeta1 -hydrogels. CONCLUSIONS: A TGFbeta1-hydrogel with appropriate biodegradability will function not only as a release matrix for the TGFbeta1, but also as a space provider for bone regeneration. The TGFbeta1-hydrogel is a promising surgical tool for skull defect repair and skull base reconstruction.
机译:目的:使用兔头骨缺损模型研究了通过转化含有生长因子-β1(TGFbeta1)的明胶水凝胶(TGFbeta1-水凝胶)诱导的颅骨再生。检查并比较了不同强度的TGFbeta1:具有固定水含量的明胶水凝胶中的不同TGFbeta1剂量,具有固定TGFbeta1剂量的明胶水凝胶中的不同水含量和溶液形式的TGFbeta1。另外,在治疗后的长时间内观察到再生的颅骨。方法:进行软X射线,双能X线吸收法和组织学研究,以评估在用TGFβ1水凝胶或其他药物治疗后,兔子的6 mm直径颅骨缺损中骨再生的时间过程。评估了TGFbeta1剂量和水凝胶水含量对TGFbeta1水凝胶对颅骨再生的影响。在治疗后6周,水含量为95 wt%的明胶水凝胶掺入了至少0.1微克的TGFbeta1,可在兔颅骨缺损部位引起明显的骨再生,而无论剂量如何,溶液形式的TGFbeta1均无效。水凝胶的体内降解性随水分含量的变化而变化,在由TGFβ1-水凝胶诱导的颅骨再生中起重要作用。在我们的水凝胶系统中,由于水凝胶降解,TGFbeta1从水凝胶中释放出来。当水凝胶降解得太快时,它不会保留TGFbeta1或阻止软组织在颅骨缺损处向内生长,并且不会在颅骨缺损处引起骨骼再生。降解速度过慢的水凝胶可能会阻碍头骨缺损处新骨的形成。用0.1微克TGFbeta1-水凝胶(95 wt%)处理后,新形成的骨头保留在缺损部位,而在6和12个月后没有被吸收。新形成的骨骼的组织学结构与正常颅骨相似。用TGFβ1-水凝胶治疗后未观察到再生骨过度生长和组织反应。结论:具有适当生物降解能力的TGFbeta1-水凝胶不仅可以用作TGFbeta1的释放基质,而且还可以作为骨再生的空间提供者。 TGFbeta1-水凝胶是用于颅骨缺损修复和颅底重建的有前途的外科工具。

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