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Preosteocytes/Osteocytes Have the Potential to Dedifferentiate Becoming a Source of Osteoblasts

机译:前骨细胞/骨细胞具有去分化成为成骨细胞来源的潜力

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摘要

Presently there is no clear evidence for the ability of mature osteogenic lineage cells to dedifferentiate. In order to identify and trace mature osteogenic lineage cells, we have utilized transgenic mouse models in which the dentin matrix protein 1 (Dmp1) promoter drives expression of GFP (active marker) or Cre recombinase (historic label) in preosteocytes/osteocytes. In long bone chip outgrowth cultures, in which cells on the bone surface were enzymatically removed, cells with previous activity of the Dmp1 promoter migrated onto plastic and down-regulated Dmp1-GFP expression. Dmp1Cre-labeled cells from these cultures had the potential to re-differentiate into the osteogenic lineage, while the negative population showed evidence of adipogenesis. We observed numerous Dmp1Cre-labeled osteoblasts on the surface of bone chips following their in vivo transplantation. Our data indicate that cells embedded in bone matrix are motile, and once given access to the extra bony milieu will migrate out of their lacunae. This population of cells is phenotypically and functionally heterogeneous in vitro. Once the preosteocytes/osteocytes leave lacunae, they can dedifferentiate, potentially providing an additional source of functional osteoblasts.
机译:目前,尚无明确证据表明成熟的成骨谱系细胞具有去分化能力。为了鉴定和追踪成熟的成骨细胞系,我们利用了转基因小鼠模型,其中牙本质基质蛋白1(Dmp1)启动子驱动前骨细胞/骨细胞中GFP(活性标记)或Cre重组酶(历史标记)的表达。在长骨芯片长出培养中,通过酶去除骨表面上的细胞,具有Dmp1启动子先前活性的细胞迁移到塑料上并下调了Dmp1-GFP表达。这些培养物中Dmp1Cre标记的细胞具有重新分化为成骨细胞谱系的潜力,而阴性群体显示出脂肪形成的迹象。我们观察到在其体内移植后,许多Dmp1Cre标记的成骨细胞在骨屑表面上。我们的数据表明,嵌入骨基质中的细胞具有运动能力,一旦获得进入额外骨质环境的通道,便会从腔隙中移出。该细胞群体在表型和功能上在体外是异质的。一旦前骨细胞/骨细胞离开腔,它们就可以去分化,从而可能提供功能性成骨细胞的其他来源。

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