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软骨缺损的基因治疗

Gene therapy for cartilage defects.

作者信息

Cucchiarini Magali, Madry Henning

机构信息

Laboratory for Experimental Orthopaedics, Department of Orthopaedic Surgery, Saarland University Medical Center, 66421 Homburg/Saar, Germany.

出版信息

J Gene Med. 2005 Dec;7(12):1495-509. doi: 10.1002/jgm.824.

Abstract

Focal defects of articular cartilage are an unsolved problem in clinical orthopaedics. These lesions do not heal spontaneously and no treatment leads to complete and durable cartilage regeneration. Although the concept of gene therapy for cartilage damage appears elegant and straightforward, current research indicates that an adaptation of gene transfer techniques to the problem of a circumscribed cartilage defect is required in order to successfully implement this approach. In particular, the localised delivery into the defect of therapeutic gene constructs is desirable. Current strategies aim at inducing chondrogenic pathways in the repair tissue that fills such defects. These include the stimulation of chondrocyte proliferation, maturation, and matrix synthesis via direct or cell transplantation-mediated approaches. Among the most studied candidates, polypeptide growth factors have shown promise to enhance the structural quality of the repair tissue. A better understanding of the basic scientific aspects of cartilage defect repair, together with the identification of additional molecular targets and the development of improved gene-delivery techniques, may allow a clinical translation of gene therapy for cartilage defects. The first experimental steps provide reason for cautious optimism.

摘要

关节软骨的局灶性缺损是临床骨科中一个尚未解决的问题。这些损伤不会自发愈合,且目前没有任何治疗方法能实现完全且持久的软骨再生。尽管软骨损伤的基因治疗概念看似简单明了,但当前研究表明,要成功实施这一方法,需要对基因转移技术进行调整以适应局限性软骨缺损问题。特别是,将治疗性基因构建体局部递送至缺损部位是很有必要的。当前策略旨在诱导填充此类缺损的修复组织中的软骨形成途径。这些策略包括通过直接或细胞移植介导的方法刺激软骨细胞增殖、成熟和基质合成。在研究最多的候选物中,多肽生长因子已显示出有望提高修复组织的结构质量。对软骨缺损修复基础科学方面的更好理解,以及额外分子靶点的识别和改进的基因递送技术的开发,可能会使软骨缺损的基因治疗实现临床转化。最初的实验步骤让人有理由谨慎乐观。

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