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掺入转化生长因子β1的脱水热交联胶原海绵修复兔颅骨缺损

Repairing of rabbit skull defect by dehydrothermally crosslinked collagen sponges incorporating transforming growth factor beta1.

作者信息

Ueda Hiroki, Nakamura Tatsuo, Yamamoto Masaya, Nagata Natsuki, Fukuda Seijun, Tabata Yasuhiko, Shimizu Yasuhiko

机构信息

Institute for Frontier Medical Sciences, Kyoto University, 53 Kawahara-cho Shogoin, Sakyo-ku, Kyoto 606-8507, Japan.

出版信息

J Control Release. 2003 Feb 14;88(1):55-64. doi: 10.1016/s0168-3659(02)00481-9.

Abstract

Collagen sponges of various biodegradabilities were prepared by dehydrothermal crosslinking at 140 degrees C for different time periods. When the collagen sponges were radioiodinated and implanted subcutaneously into the back of mice, the radioactivity remaining at the implanted site decreased with time; the longer the time of dehydrothermal crosslinking, the slower the radioactivity decrement. The radioactivity following the subcutaneous implantation of collagen sponges incorporating (125)I-labeled transforming growth factor (TGF)-beta1 also decreased with time. The time profile of both the radioactivity remainings was in good accordance to each other, irrespective of the crosslinking time. This indicates that the TGF-beta1 incorporated in the sponges was released as a result of sponge biodegradation. Potential of collagen sponges incorporating 0.1 micro g of TGF-beta1 in repairing the defect of rabbit skulls was evaluated in a stress-unloaded state. Bone repairing was induced by application of the collagen sponges incorporating 0.1 micro g of TGF-beta1 whereas that of free TGF-beta1 at the same dose and TGF-beta1-free, empty collagen sponges were ineffective. The bone defect was histologically closed by the bone tissue newly formed 6 weeks after application. Bone mineral density (BMD) analysis revealed that the collagen sponge incorporating TGF-beta1 enhanced the BMD value at the bone defect to a significantly great extent compared with other agents. A maximum enhancement of BMD was observed for the collagen sponge incorporating TGF-beta1 which was prepared by dehydrothermal crosslinking for 6 h. It was concluded that the TGF-beta1 incorporated in the collagen sponge was released in a biologically active form as a result of sponge biodegradation, resulting in enhanced bone repairing at the skull defect. It is possible that for too slowly degraded sponges, the remaining physically impairs the bone repairing at the skull defect. Induction of bone repairing would not be achieved through a rapid release of TGF-beta1 from too fast-degraded sponge.

摘要

通过在140℃下进行不同时间段的脱水热交联制备了具有不同生物降解性的胶原海绵。当胶原海绵经放射性碘化并皮下植入小鼠背部时,植入部位残留的放射性随时间降低;脱水热交联时间越长,放射性降低越慢。皮下植入含(125)I标记转化生长因子(TGF)-β1的胶原海绵后,放射性也随时间降低。无论交联时间如何,两种放射性残留的时间曲线彼此吻合良好。这表明海绵中掺入的TGF-β1是由于海绵生物降解而释放的。在无应力状态下评估了掺入0.1μg TGF-β1的胶原海绵修复兔颅骨缺损的潜力。应用掺入0.1μg TGF-β1的胶原海绵可诱导骨修复,而相同剂量的游离TGF-β1和不含TGF-β1的空胶原海绵则无效。应用6周后,骨组织在组织学上封闭了骨缺损。骨密度(BMD)分析显示,与其他制剂相比,掺入TGF-β1的胶原海绵在很大程度上提高了骨缺损处的BMD值。对于通过6小时脱水热交联制备的掺入TGF-β1的胶原海绵,观察到BMD的最大增强。得出的结论是,胶原海绵中掺入的TGF-β1由于海绵生物降解而以生物活性形式释放,从而增强了颅骨缺损处的骨修复。对于降解过慢的海绵,其残留物可能会对颅骨缺损处的骨修复产生物理损害。通过降解过快的海绵快速释放TGF-β1无法实现骨修复的诱导。

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