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转基因在动关节中的持久性和细胞更替:对慢性关节疾病基因治疗的意义。

Transgene persistence and cell turnover in the diarthrodial joint: implications for gene therapy of chronic joint diseases.

作者信息

Gouze Elvire, Gouze Jean-Noel, Palmer Glyn D, Pilapil Carmencita, Evans Christopher H, Ghivizzani Steven C

机构信息

Department of Orthopaedics and Rehabilitation, University of Florida, Gainesville, Florida 32610, USA.

出版信息

Mol Ther. 2007 Jun;15(6):1114-20. doi: 10.1038/sj.mt.6300151. Epub 2007 Apr 17.

Abstract

Local gene therapy for chronic joint diseases requires prolonged transgenic expression, but this has not been reliably achieved in animal models. Using normal and immunocompromised animals, we examined the capacity of various cell types in joint tissues to maintain and express exogenous transgenes after direct intra-articular gene delivery. We found that transgenic expression could persist for the lifetime of the animal but required precise immunological compatibility between the vector, transgene product, and host. It was not dependent on vector integration or promoter origin. We identified two phenotypically distinct sub-populations of genetically modified cells within the joint: (i) transient cells, with a half-life of a few weeks, and (ii) stable cells that reside in the joint tissues indefinitely. Contrary to the prevailing assumption, the transient sub-population was composed almost exclusively of synovial fibroblasts, indicating that the synovium is not an appropriate tissue upon which to base a long-term therapy. Instead, fibroblasts in the ligaments, tendons, and capsule emerged as the primary cell types capable of sustained therapeutic transgene expression. This study sheds new light on the cellular dynamics of articular tissues and suggests that cell turnover and immune reactivity are the key determinants in achieving sustained transgenic expression intra-articularly.

摘要

慢性关节疾病的局部基因治疗需要长期的转基因表达,但在动物模型中尚未可靠地实现这一点。我们使用正常和免疫受损动物,研究了关节组织中各种细胞类型在直接关节内基因递送后维持和表达外源转基因的能力。我们发现转基因表达可以在动物的一生中持续存在,但需要载体、转基因产物和宿主之间精确的免疫相容性。它不依赖于载体整合或启动子来源。我们在关节内鉴定出两个表型不同的转基因修饰细胞亚群:(i)半衰期为数周的短暂细胞,以及(ii)无限期驻留在关节组织中的稳定细胞。与普遍的假设相反,短暂亚群几乎完全由滑膜成纤维细胞组成,这表明滑膜不是长期治疗的合适组织。相反,韧带、肌腱和关节囊中的成纤维细胞成为能够持续表达治疗性转基因的主要细胞类型。这项研究为关节组织的细胞动力学提供了新的见解,并表明细胞更新和免疫反应性是在关节内实现持续转基因表达的关键决定因素。

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