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使用负载有表达 BMP-7 的原代软骨细胞的冷冻凝胶支架进行耳廓软骨修复。

Auricular cartilage repair using cryogel scaffolds loaded with BMP-7-expressing primary chondrocytes.

机构信息

Chemical Engineering Department and Bioengineering Division and Centre for Bioengineering (Biyomedtek), Hacettepe University, Beytepe, Ankara, Turkey.

出版信息

J Tissue Eng Regen Med. 2013 Oct;7(10):831-40. doi: 10.1002/term.1634. Epub 2012 Dec 26.

Abstract

The loss of cartilage tissue due to trauma, tumour surgery or congenital defects, such as microtia and anotia, is one of the major concerns in head and neck surgery. Recently tissue-engineering approaches, including gene delivery, have been proposed for the regeneration of cartilage tissue. In this study, primary chondrocytes were genetically modified with plasmid-encoding bone morphogenetic protein-7 (BMP-7) via the commercially available non-viral Turbofect vector, with the aim of bringing ex vivo transfected chondrocytes to resynthesize BMP-7 in vitro as they would in vivo. Genetically modified cells were implanted into gelatin-oxidized dextran scaffolds and cartilage tissue formation was investigated in 15 × 15 mm auricular cartilage defects in vivo in 48 New Zealand (NZ) white rabbits for 4 months. The results were evaluated via histology and early gene expression. Early gene expression results indicated a strong effect of exogenous BMP-7 on matrix synthesis and chondrocyte growth. In addition, histological analysis results exhibited significantly better cartilage healing with BMP-7-modified (transfected) cells than in the non-modified (non-transfected) group and as well as the control.

摘要

由于创伤、肿瘤手术或先天性缺陷(如小耳畸形和无耳畸形)导致的软骨组织丧失是头颈部外科的主要关注点之一。最近,包括基因传递在内的组织工程方法已被提出用于软骨组织的再生。在这项研究中,通过市售的非病毒 Turbofect 载体,用编码骨形态发生蛋白 7(BMP-7)的质粒对原代软骨细胞进行基因修饰,目的是使体外转染的软骨细胞在体外重新合成 BMP-7,就像在体内一样。将基因修饰的细胞植入氧化明胶化葡聚糖支架中,并在 48 只新西兰(NZ)白兔的 15×15mm 耳廓软骨缺损中进行了为期 4 个月的体内研究。通过组织学和早期基因表达评估结果。早期基因表达结果表明,外源性 BMP-7 对基质合成和软骨细胞生长有很强的影响。此外,组织学分析结果表明,BMP-7 修饰(转染)细胞的软骨愈合明显优于未修饰(未转染)组和对照组。

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