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缺氧促进人骨髓间充质干细胞的增殖和成骨分化潜能。

Hypoxia promotes proliferation and osteogenic differentiation potentials of human mesenchymal stem cells.

机构信息

Institute of Clinical Medicine, National Yang-Ming University, Taipei, Taiwan.

出版信息

J Orthop Res. 2012 Feb;30(2):260-6. doi: 10.1002/jor.21517. Epub 2011 Aug 1.

Abstract

Mesenchymal stem cells (MSCs), which can be isolated from bone marrow and other somatic tissues, are residing in an environment with relative low oxygen tension. The purpose of this study is to investigate the effects of hypoxia on MSCs, and we hypothesize that oxygen concentration regulates the intricate balance between cellular proliferation and commitment towards differentiation. In this study, human bone marrow-derived MSCs were cultured under hypoxia with 1% O(2). The proliferation ability of MSCs was increased after a 7-day hypoxic culture period. Migration assay showed that hypoxia enhanced the migration capabilities of MSCs. Moreover, expression of stemness genes Oct4, Nanog, Sall4 and Klf4 was increased under hypoxia. Furthermore, the differentiation ability of MSCs under hypoxia favored osteogenesis while adipogenesis was inhibited during a 4-week induction period. Cytokine antibody array analysis showed that a number of growth factors were up-regulated after a 7-day hypoxic incubation and the differential expression of growth factors may account for the increased proliferation and osteogenic potentials of MSCs under hypoxic condition. Taken together, hypoxia provides a favorable culture condition to promote proliferation as well as osteogenesis of MSCs through differential growth factor production.

摘要

间充质干细胞(MSCs)可从骨髓和其他体细胞组织中分离出来,它们存在于相对低氧张力的环境中。本研究旨在探讨低氧对 MSCs 的影响,我们假设氧浓度调节细胞增殖和向分化方向分化之间的精细平衡。在这项研究中,人骨髓来源的 MSCs 在 1%O(2)的低氧条件下培养。经过 7 天的低氧培养,MSCs 的增殖能力增加。迁移实验表明低氧增强了 MSCs 的迁移能力。此外,低氧下干细胞基因 Oct4、Nanog、Sall4 和 Klf4 的表达增加。此外,在 4 周的诱导期内,低氧下 MSCs 的分化能力有利于成骨,而抑制脂肪生成。细胞因子抗体阵列分析显示,7 天低氧孵育后,大量生长因子上调,生长因子的差异表达可能是低氧条件下 MSCs 增殖和成骨潜能增加的原因。综上所述,低氧通过差异生长因子的产生为促进 MSCs 的增殖和成骨提供了有利的培养条件。

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