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基因激活组织移植物用于持续的骨形态发生蛋白-2 递送和骨工程:带筋膜的肌肉优于肌肉和脂肪吗?

Gene-activated tissue grafts for sustained bone morphogenetic protein-2 delivery and bone engineering: Is muscle with fascia superior to muscle and fat?

机构信息

Department of Orthopedic Surgery, Physical Medicine and Rehabilitation, University Hospital Grosshadern, Ludwig-Maximilians-University Munich, Munich, Germany.

Sirion Biotech GmbH, Martinsried, Germany.

出版信息

J Tissue Eng Regen Med. 2018 Apr;12(4):1002-1011. doi: 10.1002/term.2575. Epub 2017 Nov 22.

DOI:10.1002/term.2575
PMID:28940796
Abstract

Previously, we have presented an expedited strategy for sustained delivery of bone morphogenetic protein-2 (BMP-2) to bone lesions based on the implantation of gene-activated fat and muscle fragments. The aim of the present in vitro experiments was to evaluate the potential of muscle with fascia as a BMP-2 delivering osteo-regenerative implant in comparison to fat tissue and muscle alone. Subcutaneous fat, muscle, and muscle with fascia were harvested from Fischer 344 rats. The tissues were cut into small pieces and cultured for up to 90 days after direct transduction with adenoviral BMP-2 or green fluorescence protein vectors. Different vector doses were applied, and proliferation, long-term BMP-2 production, and osteogenic differentiation of the 3 different tissues were investigated in vitro. Muscle with fascia produced the largest amounts of BMP-2. Expression of the transgene was detected for up to 90 days. Proliferation was reduced with increased vector doses. Muscle with fascia showed a higher potential for osteogenic differentiation than fat, but it was not improved as compared to muscle alone. A dose of 4 × 10 plaque forming units of the adenoviral BMP-2 vector appeared to be the optimal dose for transduction of muscle with fascia. Because muscle with fascia produced higher amounts of BMP-2 as compared to muscle alone or fat tissue grafts, showing a high potential for osteogenic differentiation, it might represent an improved osteo-regenerative implant facilitating endogenous repair. Future studies should investigate the effect of muscle with fascia transduced with 4 × 10 plaque forming units on bone healing in vivo.

摘要

先前,我们提出了一种基于基因激活脂肪和肌肉碎片植入的加速骨形态发生蛋白-2(BMP-2)持续递送至骨病变的策略。本体外实验的目的是评估筋膜肌肉作为 BMP-2 传递骨再生植入物的潜力,与单独的脂肪组织和肌肉进行比较。从 Fischer 344 大鼠中采集皮下脂肪、肌肉和筋膜肌肉。将这些组织切成小块,在直接转导腺病毒 BMP-2 或绿色荧光蛋白载体后培养长达 90 天。应用不同的载体剂量,研究了 3 种不同组织的增殖、长期 BMP-2 产生和成骨分化的体外情况。筋膜肌肉产生了最大量的 BMP-2。转导基因的表达可检测长达 90 天。随着载体剂量的增加,增殖减少。筋膜肌肉的成骨分化潜力高于脂肪,但与单独的肌肉相比没有提高。腺病毒 BMP-2 载体的 4×10 噬菌斑形成单位的剂量似乎是转导筋膜肌肉的最佳剂量。由于筋膜肌肉产生的 BMP-2 比单独的肌肉或脂肪组织移植物多,显示出较高的成骨分化潜力,因此它可能代表一种改进的骨再生植入物,促进内源性修复。未来的研究应研究 4×10 噬菌斑形成单位转导的筋膜肌肉对体内骨愈合的影响。

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