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负载骨形态发生蛋白-7的聚乙交酯丙交酯微球作为一种新型递送系统用于在I型胶原凝胶中培养人软骨细胞:普通裸鼠模型

BMP-7-loaded PGLA microspheres as a new delivery system for the cultivation of human chondrocytes in a collagen type I gel: the common nude mouse model.

作者信息

Gavenis Karsten, Schneider Ulrich, Groll Jürgen, Schmidt-Rohlfing Bernhard

机构信息

Department of Orthopedic and Trauma Surgery, Aachen University Hospital, Aachen, Germany.

出版信息

Int J Artif Organs. 2010 Jan;33(1):45-53.

Abstract

PURPOSE

Bone morphogenic protein 7 (BMP-7) released from polylactide (PLGA) microspheres has proven to be a potent system in cartilage tissue engineering in vitro. However, in vivo data are still lacking. The aim of this study was to investigate this BMP-7 release system utilizing the nude mouse as a small animal model.

METHODS

Human osteoarthritic chondrocytes of 10 patients were enzymatically released and transferred into a collagen type-I gel. A concentration of 2x10(5) cells/mL was used. BMP-7 encapsulated in PGLA microspheres was added at an initial concentration of 500 ng BMP-7/mL gel. Untreated specimens and specimens with empty microspheres served as control. Samples were cultivated subcutaneously in nude mice for 6 weeks.

RESULTS

After recovery, chondrocytes of all groups displayed a spheroid morphology without signs of dedifferentiation. The proteoglycan and collagen type II content of the control groups was restricted to the immediate pericellular region, whereas treatment group samples showed enhanced collagen type II production. Collagen type II and aggrecan gene expression was enhanced in treatment group samples with respect to the two control groups (mean +/- SD: 0.268 +/- 0.450 to 0.152 +/- 0.129 and 0.155 +/- 0.216 ng/ng beta-actin for collagen type II; 0.535 +/- 0.731 to 0.367 +/- 0.651 and 0.405 +/- 0.326 ng/ng beta-actin for aggrecan), whereas collagen type I gene expression decreased by a factor of 10. Relative protein quantification of collagen type II, collagen type I and proteoglycan was in accordance.

CONCLUSIONS

Our data suggest that BMP-7 release from PGLA microspheres led to an improved tissue-engineered cartilage analogue in vivo with an increase in hyaline-cartilage-specific components.

摘要

目的

从聚丙交酯(PLGA)微球释放的骨形态发生蛋白7(BMP - 7)已被证明在体外软骨组织工程中是一种有效的体系。然而,体内数据仍然缺乏。本研究的目的是利用裸鼠作为小动物模型来研究这种BMP - 7释放系统。

方法

将10例患者的人骨关节炎软骨细胞通过酶解分离并转移到I型胶原凝胶中。使用的细胞浓度为2×10⁵个细胞/毫升。以500 ng BMP - 7/毫升凝胶的初始浓度加入封装在PGLA微球中的BMP - 7。未处理的标本和含有空微球的标本作为对照。样品在裸鼠皮下培养6周。

结果

回收后,所有组的软骨细胞均呈现球状形态,无去分化迹象。对照组的蛋白聚糖和II型胶原含量局限于紧邻细胞周围区域,而治疗组样品显示II型胶原产生增加。与两个对照组相比,治疗组样品中II型胶原和聚集蛋白聚糖基因表达增强(II型胶原:平均值±标准差为0.268±0.450至0.152±0.129以及0.155±0.216 ng/ng β -肌动蛋白;聚集蛋白聚糖:0.535±0.731至0.367±0.651以及0.405±0.326 ng/ng β -肌动蛋白),而I型胶原基因表达下降了10倍。II型胶原、I型胶原和蛋白聚糖的相对蛋白定量结果一致。

结论

我们的数据表明,PGLA微球释放的BMP - 7在体内导致组织工程软骨类似物得到改善,透明软骨特异性成分增加。

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