Oxygen tension directs chondrogenic differentiation of myelo-monocytic progenitors during endochondral bone formation.

Jessica Shafer, Alan R Davis, Francis H Gannon, Christine M Fouletier-Dilling, Zawaunyka Lazard, Kevin Moran, Zbigniew Gugala, Mustafa Ozen, Michael Ittmann, Michael H Heggeness, Elizabeth Olmsted-Davis
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引用次数: 19

Abstract

Synthesis of bone requires both essential progenitors to form the various structures and the correct microenvironment for their differentiation. To identify these factors, we have used a system that exploits bone morphogenetic protein's ability to induce endochondral bone formation rapidly. One of the earliest events observed was the influx and proliferation of fibroblastic cells that express both vascular smooth muscle cell markers, alpha smooth muscle actin (alpha SMA), smooth muscle myosin heavy chain, and the monocytic marker CD68. The expression of these factors was lost by days 4 to 5, coincident with the up-regulation of Sox9 and the appearance of chondrocytes. Studies with a cyclization recombination (Cre)/lox system, in which a myeloid-specific promoter driving Cre recombinase can irreversibly unblock expression of beta-galactosidase only in cells of myeloid origin, showed specific activity in the newly formed chondrocytes. These results suggest that early chondrocyte progenitors are of myeloid origin. Simultaneous with this recruitment, we determined that a numbers of these cells were in a hypoxic state, indicative of a low-oxygen environment. The cells in the hypoxic regions were undergoing chondrogenesis, whereas cells in adjacent normoxic regions appeared to be assembling into new vessels, suggesting that the oxygen microenvironment is critical for establishment of the cartilage.

在软骨内骨形成过程中,氧张力指导骨髓单核细胞祖细胞的软骨分化。
骨的合成既需要形成各种结构的基本祖细胞,也需要它们分化的正确微环境。为了确定这些因素,我们使用了一个系统,利用骨形态发生蛋白快速诱导软骨内骨形成的能力。最早观察到的事件之一是纤维母细胞的涌入和增殖,这些细胞表达血管平滑肌细胞标记物,α平滑肌肌动蛋白(α SMA),平滑肌肌球蛋白重链和单核细胞标记物CD68。这些因子的表达在第4 ~ 5天消失,与Sox9的上调和软骨细胞的出现一致。在环化重组(Cre)/lox系统中,髓系特异性启动子驱动Cre重组酶只能在髓系起源的细胞中不可逆地解除β -半乳糖苷酶的表达,在新形成的软骨细胞中显示出特异性活性。这些结果提示早期软骨细胞祖细胞起源于髓系。与此同时,我们确定这些细胞中的许多处于缺氧状态,表明低氧环境。缺氧区的细胞正在发生软骨形成,而邻近常氧区的细胞似乎正在组装成新的血管,这表明氧微环境对软骨的形成至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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Tissue engineering
Tissue engineering CELL & TISSUE ENGINEERING-BIOTECHNOLOGY & APPLIED MICROBIOLOGY
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