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椎间盘细胞的多样性:表型与功能。

Diversity of intervertebral disc cells: phenotype and function.

机构信息

AO Research Institute Davos, Switzerland.

出版信息

J Anat. 2012 Dec;221(6):480-96. doi: 10.1111/j.1469-7580.2012.01521.x. Epub 2012 Jun 11.

Abstract

The intervertebral disc (IVD) is a moderately moving joint that is located between the bony vertebrae and provides flexibility and load transmission throughout the spinal column. The disc is composed of different but interrelated tissues, including the central highly hydrated nucleus pulposus (NP), the surrounding elastic and fibrous annulus fibrosus (AF), and the cartilaginous endplate (CEP), which provides the connection to the vertebral bodies. Each of these tissues has a different function and consists of a specific matrix structure that is maintained by a cell population with distinct phenotype. Although the healthy IVD is able to balance the slow matrix turnover of synthesis and degradation, this balance is often disturbed, leading to degenerative disorders. Successful therapeutic management of IVD degeneration requires a profound understanding of the cellular and molecular characteristics of the functional IVD. Hence, the phenotype of IVD cells has been of significant interest from multiple perspectives, including development, growth, remodelling, degeneration and repair. One major challenge that complicates our understanding of the disc cells is that both the cellular phenotype and the extracellular matrix strongly depend on disc maturity and health and as a consequence are continuously evolving. This review delineates the diversity of the cell types found in the intervertebral disc, with emphasis on human, but with reference to other species. The cells of the NP appear rounded and express a proteoglycan-rich matrix, whereas the more elongated AF cells are embedded in a collagen fibre matrix and the CEPs represent a layer of cartilage. Even though all disc cells have often been referred to as 'intervertebral disc chondrocytes', distinct phenotypical differences in comparison with articular chondrocytes exist and have been reported recently. The availability of more specific markers has also improved our understanding of progenitor cell differentiation towards an IVD cell phenotype. Ultimately, new cell- and tissue-engineering approaches to regenerative therapies will only be successful if the specific characteristics of the individual tissues and their context in the function of the whole organ, are taken into consideration.

摘要

椎间盘(IVD)是一种中度活动关节,位于骨椎骨之间,为脊柱提供灵活性和载荷传递。椎间盘由不同但相互关联的组织组成,包括中央高度水合的髓核(NP)、周围有弹性和纤维的纤维环(AF)以及软骨终板(CEP),它们为椎体提供连接。这些组织中的每一个都有不同的功能,由特定的基质结构组成,由具有不同表型的细胞群体维持。尽管健康的椎间盘能够平衡合成和降解的缓慢基质转化,但这种平衡经常被打乱,导致退行性疾病。成功治疗椎间盘退变需要深刻理解功能性椎间盘的细胞和分子特征。因此,椎间盘细胞的表型一直受到多方面的关注,包括发育、生长、重塑、退变和修复。一个使我们对椎间盘细胞的理解变得复杂的主要挑战是,细胞表型和细胞外基质强烈依赖于椎间盘的成熟度和健康状况,因此它们在不断演变。这篇综述阐述了在椎间盘中发现的细胞类型的多样性,重点是人类,但也参考了其他物种。NP 中的细胞呈圆形,表达富含蛋白聚糖的基质,而更细长的 AF 细胞则嵌入在胶原纤维基质中,CEP 代表一层软骨。尽管所有椎间盘细胞通常都被称为“椎间盘软骨细胞”,但与关节软骨细胞相比,它们在表型上存在明显差异,最近已经有报道。更多特异性标记物的可用性也提高了我们对祖细胞向椎间盘细胞表型分化的理解。最终,如果不考虑各个组织的特定特征及其在整个器官功能中的背景,新的细胞和组织工程方法再生疗法将不会成功。

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