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通过从由明胶和β-磷酸三钙组成的可生物降解海绵中控制释放骨形态发生蛋白-2增强骨诱导作用。

Enhanced osteoinduction by controlled release of bone morphogenetic protein-2 from biodegradable sponge composed of gelatin and beta-tricalcium phosphate.

作者信息

Takahashi Yoshitake, Yamamoto Masaya, Tabata Yasuhiko

机构信息

Department of Biomaterials, Field of Tissue Engineering, Institute for Frontier Medical Sciences, Kyoto University, 53 Kawara-cho Shogoin, Sakyo-ku, Kyoto 606-8507, Japan.

出版信息

Biomaterials. 2005 Aug;26(23):4856-65. doi: 10.1016/j.biomaterials.2005.01.012.

Abstract

Biodegradable gelatin sponges at different contents of beta-tricalcium phosphate (beta-TCP) were fabricated to allow bone morphogenetic protein (BMP)-2 to incorporate into them. The in vivo osteoinduction activity of the sponges incorporating BMP-2 was investigated, while their in vivo profile of BMP-2 release was evaluated. The sponges prepared had an interconnected pore structure with an average pore size of 200 microm, irrespective of the beta-TCP content. The in vivo release test revealed that BMP-2 was released in vivo at a similar time profile, irrespective of the beta-TCP content. The in vivo time period of BMP-2 retention was longer than 28 days. When the osteoinduction activity of gelatin or gelatin-beta-TCP sponges incorporating BMP-2 was studied following the implantation into the back subcutis of rats in terms of histological and biochemical examinations, homogeneous bone formation was histologically observed throughout the sponges, although the extent of bone formation was higher in the sponges with the lower contents of beta-TCP. On the other hand, the level of alkaline phosphatase activity and osteocalcin content at the implanted sites of sponges decreased with an increase in the content of beta-TCP. The gelatin sponge exhibited significantly higher osteoinduction activity than that of any gelatin-beta-TCP sponge, although every sponge with or without beta-TCP showed a similar in vivo profile of BMP-2 release. In addition, the in vitro collagenase digestion experiments revealed that the gelatin-beta-TCP sponge collapsed easier than the gelatin sponge without beta-TCP incorporation. These results suggest that the maintenance of the intrasponge space necessary for the osteoinduction is one factor contributing to the osteoinduction extent of BMP-2-incorporating sponges.

摘要

制备了不同β-磷酸三钙(β-TCP)含量的可生物降解明胶海绵,以使骨形态发生蛋白(BMP)-2能够掺入其中。研究了掺入BMP-2的海绵的体内骨诱导活性,同时评估了它们体内BMP-2的释放情况。所制备的海绵具有相互连通的孔结构,平均孔径为200微米,与β-TCP含量无关。体内释放试验表明,无论β-TCP含量如何,BMP-2在体内以相似的时间模式释放。BMP-2在体内保留的时间段超过28天。当通过组织学和生化检查研究将掺入BMP-2的明胶或明胶-β-TCP海绵植入大鼠背部皮下后的骨诱导活性时,在整个海绵中组织学观察到均匀的骨形成,尽管β-TCP含量较低的海绵中骨形成的程度更高。另一方面,海绵植入部位的碱性磷酸酶活性水平和骨钙素含量随着β-TCP含量的增加而降低。尽管每种含或不含β-TCP的海绵在体内都显示出相似的BMP-2释放情况,但明胶海绵表现出比任何明胶-β-TCP海绵更高的骨诱导活性。此外,体外胶原酶消化实验表明,明胶-β-TCP海绵比未掺入β-TCP的明胶海绵更容易塌陷。这些结果表明,骨诱导所需的海绵内空间的维持是影响掺入BMP-2的海绵骨诱导程度的一个因素。

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