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Gene therapy applications in orthopaedics.

机译:基因治疗在骨科中的应用。

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With great interest and enthusiasm, we read the article "Orthopaedic applications of gene therapy" . The authors should be congratulated for their concise yet very thorough and excellent coverage of the gene therapy applications in orthopaedics. However, it is our opinion that articular cartilage deserved more of their attention. Primarily, we think that the subsection heading "Cartilage repair" should be expanded to "Cartilage repair and regeneration", particularly since the authors did mention "stimulation of cartilage regeneration" which implies the possibility of inducing intrinsic healing of the damaged cartilage by hyaline cartilage formation. When treating localised cartilage defects we should ask ourselves: What kind of new tissue formation inside the defect do we want to induce? Ideally we aim for articular cartilage regeneration, not repair, which would mean formation of hyaline cartilage, not fibrocartilage. Treatment options published in the literature can be roughly divided into two concepts-reparative and restorative. The end result of the first concept is fibrocartilage, and the microfracture technique is the most popular representative. In contrast, the restorative concept aims for hyaline cartilage implantation/formation and includes implantation of osteochondral plugs with perfectly organised cartilage and matrix and/or cell therapy,namely autologous chondrocyte transplantation. Anabolic factors including members of the TGF-beta superfamily, such as BMPs, have proven their potential to stimulate chondrogenesis and synthesis of cartilage-specific matrix components in animal models [2, 3]. However, those proteins have short half-lives and it is difficult to maintain adequate in situ concentrations necessary for their proper functioning. Furthermore, many proteins act intracellularly and because cells cannot normally import these proteins, they cannot be used in soluble forms. These problems are the reason why gene therapy has attracted so much attention lately. The transfer of the respective genes into the joint, possibly in combination with the supply of chondroprogenitor cells, might be an elegant method to achieve a sustained delivery of such therapeutic factors at the required location in vivo . Pascher et al. developed a novel ex vivo method by using coagulated bone marrow aspirate as a mean of gene delivery to cartilage. Vector-seeded and cell-seeded bone marrow clots ("gene plugs") were found to maintain their structural integrity following extensive culture and maintained transgenic expression for several weeks.
机译:我们怀着极大的兴趣和热情阅读了“基因治疗的骨科应用”一文。应该为作者对骨科中基因治疗应用的简洁却非常全面和出色的覆盖面表示祝贺。但是,我们认为关节软骨值得更多关注。首先,我们认为标题为“软骨修复”的小节应扩展为“软骨修复和再生”,特别是因为作者确实提到了“刺激软骨再生”,这暗示有可能通过透明软骨诱导受损软骨的内在愈合。编队。在治疗局部软骨缺损时,我们应该问自己:我们要在缺损内诱导什么样的新组织形成?理想情况下,我们的目标是关节软骨再生,而不是修复,这意味着形成透明软骨而不是纤维软骨。文献中发表的治疗方案可以大致分为两个概念:修复性和修复性。第一个概念的最终结果是纤维软骨,而微骨折技术是最受欢迎的代表。相比之下,修复概念旨在透明软骨的植入/形成,包括植入具有完美组织的软骨和基质和/或细胞疗法的骨软骨栓,即自体软骨细胞移植。包括TGF-β超家族成员(如BMP)在内的合成代谢因子已被证明具有刺激动物模型中软骨形成和软骨特异性基质成分合成的潜力[2,3]。然而,这些蛋白质的半衰期短,并且难以维持适当的原位浓度以维持其正常功能。此外,许多蛋白质在细胞内起作用,并且由于细胞通常不能导入这些蛋白质,因此它们不能以可溶形式使用。这些问题是最近基因治疗引起如此多关注的原因。将各自的基因转移到关节中,可能与软骨生成细胞的供应结合在一起,可能是一种在体内所需位置持续递送此类治疗因子的简便方法。 Pascher等。通过使用凝结的骨髓穿刺液作为将基因传递到软骨的一种新方法,开发了一种新颖的离体方法。发现在大量培养后,带有载体的和具有细胞的骨髓凝块(“基因栓”)保持其结构完整性,并保持转基因表达数周。

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