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腰椎间盘基因传递:Lewis 大鼠的初步研究。

Lumbar spine intervertebral disc gene delivery: a pilot study in lewis rats.

机构信息

Hospital for Special Surgery, 535 East 70th Street, New York, NY 10021 USA.

Hospital for Special Surgery, 535 East 70th Street, New York, NY 10021 USA ; Weill Cornell Medical College, New York, NY 10065 USA.

出版信息

HSS J. 2013 Feb;9(1):36-41. doi: 10.1007/s11420-012-9319-3. Epub 2013 Jan 8.

Abstract

BACKGROUND

Basic research toward understanding and treating disc pathology in the spine has utilized numerous animal models, with delivery of small molecules, purified factors, and genes of interest. To date, gene delivery to the rat lumbar spine has only been described utilizing genetically programmed cells in a matrix which has required partial disc excision, and expected limitation of treatment diffusion into the disc.

PURPOSE

This study was designed to develop and describe a surgical technique for lumbar spine exposure and disc space preparation, and use of a matrix-free method for gene delivery.

METHODS

Naïve or genetically programmed isogeneic bone marrow stromal cells were surgically delivered to adolescent male Lewis rat lumbar discs, and utilizing quantitative biochemical and qualitative immunohistological assessments, the implanted cells were detected 3 days post-procedure.

RESULTS

Statistically significant differences were noted for recovery of the β-galactosidase marker gene comparing delivery of naïve or labeled cells (10(5) cells per disc) from the site of implantation, and between delivery of 10(5) or 10(6) labeled cells per disc at the site of implantation and the adjacent vertebral body. Immunohistology confirmed that the β-galactosidase marker was detected in the adjacent vertebra bone in the zone of surgical implantation.

CONCLUSIONS

The model requires further testing in larger cohorts and with biologically active genes of interest, but the observations from the pilot experiments are very encouraging that this will be a useful comparative model for basic spine research involving gene or cell delivery, or other locally delivered therapies to the intervertebral disc or adjacent vertebral bodies in rats.

摘要

背景

为了理解和治疗脊柱椎间盘病变,基础研究已经利用了许多动物模型,包括小分子、纯化因子和感兴趣的基因的递送。迄今为止,向大鼠腰椎递送基因仅通过在基质中编程的遗传细胞来描述,这需要部分椎间盘切除,并预计治疗扩散到椎间盘的限制。

目的

本研究旨在开发和描述一种用于腰椎暴露和椎间盘间隙准备的手术技术,并使用无基质方法进行基因递送。

方法

幼稚或基因编程的同种异体骨髓基质细胞通过手术递送至未成年雄性 Lewis 大鼠腰椎间盘,并利用定量生化和定性免疫组织化学评估,在术后 3 天检测到植入的细胞。

结果

从植入部位递送幼稚或标记细胞(每个椎间盘 10(5)个细胞)以及从植入部位递送 10(5)个或 10(6)个标记细胞与相邻椎体之间,β-半乳糖苷酶标记基因的回收存在统计学显著差异。免疫组织化学证实,β-半乳糖苷酶标记在手术植入区的相邻椎骨中被检测到。

结论

该模型需要在更大的队列和具有生物活性的感兴趣基因中进行进一步测试,但初步实验的观察结果非常令人鼓舞,这将是一个有用的比较模型,用于涉及基因或细胞递送或其他局部递送到大鼠椎间盘或相邻椎体的基础脊柱研究。

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