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骨形态发生蛋白-9 或其衍生肽递送系统诱导异位骨形成的评价。

The evaluation of ectopic bone formation induced by delivery systems for bone morphogenetic protein-9 or its derived peptide.

机构信息

Laboratory of Cell-Biomaterial Biohybrid Systems, Department of Chemical Engineering and Biotechnological Engineering, Faculty of Engineering, Université de Sherbrooke, Sherbrooke, Québec, Canada.

出版信息

Tissue Eng Part A. 2012 Feb;18(3-4):342-52. doi: 10.1089/ten.TEA.2011.0008. Epub 2011 Oct 26.

Abstract

We have earlier shown that a peptide derived from the bone morphogenetic protein-9 (pBMP-9) stimulates mouse preosteoblasts MC3T3-E1 differentiation in vitro. Here, we evaluated the effects of two delivery systems (DSs) for pBMP-9, one based on collagen and the other on chitosan. The release kinetics of BMP-9 (used as control) and pBMP-9 from these DSs were first determined in vitro by using enzyme-linked immunosorbent assay and high performance liquid chromatography assays, respectively. Micro-computerized tomography and histological analysis were then performed to study in vivo the ectopic ossification induced by both DSs containing these molecules in C57BL/6 mouse quadriceps. We found that collagen DS released in vitro about 35% of its BMP-9 within 1 h, whereas chitosan DS released 80%. The pBMP-9 was released from both DSs more slowly for up to 10 days. These release kinetics seemed to fit the Korsmeyer-Peppas model. Only chitosan DS containing BMP-9 induced strong bone formation in all mice quadriceps within 24 days. All mice quadriceps treated by pBMP-9 trapped in this DS also favored bone structures that started to mineralize. However, pBMP-9 in collagen DS failed to promote ectopic ossification within 24 days in vivo. This study highlights the importance to optimize carrier, thus improving the efficiency of pBMP-9 in vivo.

摘要

我们之前已经证明,骨形态发生蛋白 9(BMP-9)的一种肽段可以刺激体外小鼠前成骨细胞 MC3T3-E1 的分化。在这里,我们评估了两种 BMP-9 传递系统(DS)的效果,一种基于胶原蛋白,另一种基于壳聚糖。首先通过酶联免疫吸附试验和高效液相色谱法分别在体外测定 BMP-9(用作对照)和这些 DS 中 pBMP-9 的释放动力学。然后通过 micro-CT 和组织学分析研究这两种 DS 中这些分子在 C57BL/6 小鼠四头肌中异位成骨的情况。我们发现胶原蛋白 DS 在体外 1 小时内释放了约 35%的 BMP-9,而壳聚糖 DS 释放了 80%。pBMP-9 从这两种 DS 中释放的速度较慢,持续长达 10 天。这些释放动力学似乎符合 Korsmeyer-Peppas 模型。只有含有 BMP-9 的壳聚糖 DS 在 24 天内诱导了所有小鼠四头肌的强烈骨形成。在这种 DS 中被 pBMP-9 捕获的所有小鼠四头肌也有利于开始矿化的骨结构。然而,在体内 24 天内,胶原蛋白 DS 中的 pBMP-9 未能促进异位骨化。这项研究强调了优化载体的重要性,从而提高了 pBMP-9 的体内效率。

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