首页> 外文期刊>European spine journal: official publication of the European Spine Society, the European Spinal Deformity Society, and the European Section of the Cervical Spine Research Society >An understanding of intervertebral disc development, maturation and cell phenotype provides clues to direct cell-based tissue regeneration therapies for disc degeneration
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An understanding of intervertebral disc development, maturation and cell phenotype provides clues to direct cell-based tissue regeneration therapies for disc degeneration

机译:对椎间盘发育,成熟和细胞表型的了解为直接基于细胞的组织再生疗法进行椎间盘退变提供了线索

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Abstract Cell-based regenerative medicine therapies have been proposed for repairing the degenerated intervertebral disc (a major cause of back pain). However, for this approach to be successful, it is essential to characterise the phenotype of its native cells to guarantee that implanted cells differentiate and maintain the correct phenotype to ensure appropriate cell and tissue function. While recent studies have increased our knowledge of the human nucleus pulposus (NP) cell phenotype, their ontogeny is still unclear. The expression of notochordal markers by a subpopulation of adult NP cells suggests that, contrary to previous reports, notochord-derived cells are retained in the adult NP, possibly coexisting with a second population of cells originating from the annulus fibrosus or endplate. It is not known, however, how these two cell populations interact and their specific role(s) in disc homeostasis and disease. In particular, notochordal cells are proposed to display both anabolic and protective roles; therefore, they may be the ideal cells to repair the degenerate disc. Thus, understanding the ontogeny of the adult NP cells is paramount, as it will inform the medical and scientific communities as to the ideal phenotype to implant into the degenerate disc and the specific pathways involved in stem cell differentiation towards such a phenotype.
机译:摘要已经提出了基于细胞的再生医学疗法,以修复退化的椎间盘(背痛的主要原因)。但是,要使该方法成功,必须表征其天然细胞的表型,以确保植入的细胞分化并维持正确的表型,以确保适当的细胞和组织功能。虽然最近的研究增加了我们对人类髓核(NP)细胞表型的了解,但它们的个体发育仍不清楚。由成年NP细胞亚群表达的脊索标记表明,与以前的报道相反,成年NP中保留了由脊索衍生的细胞,可能与源自纤维环或终板的第二批细胞共存。但是,尚不清楚这两个细胞群如何相互作用以及它们在椎间盘稳态和疾病中的特定作用。特别地,提出了脊索细胞显示出同化和保护作用。因此,它们可能是修复退化光盘的理想细胞。因此,了解成年NP细胞的个体发育至关重要,因为它将告知医学和科学界关于植入退化的椎间盘的理想表型以及干细胞向该表型分化的具体途径。

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