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Matrix stiffness determines the fate of nucleus pulposus-derived stem cells

机译:基质硬度决定了髓核衍生干细胞的命运

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Intervertebral disc (IVD) degeneration and consequent low-back pain present a major medical challenge. Nucleus pulposus-derived stem cells (NP-SCs) may lead to a novel therapy for this severe disease. It was recently shown that survival and function of mature NP cells are regulated in part by tissue stiffness. We hypothesized that modification of matrix stiffness will influence the ability of cultured NP-SCs to proliferate, survive, and differentiate into mature NP cells. NP-SCs were subcultured in threedimensional matrices of varying degrees of stiffness as measured by the material's shear storage modulus. Cell survival, activity, and rate of differentiation toward the chondrogenic or osteogenic lineage were analyzed. NP-SCs were found to proliferate and differentiate in all matrices, irrespective of matrix stiffness. However, matrices with a low shear storage modulus (G' = 1 kPa) promoted significantly more proliferation and chondrogenic differentiation, whereas matrices with a high modulus (G' = 2 kPa) promoted osteogenic differentiation. Imaging performed via confocal and scanning electron microscopes validated cell survival and highlighted stiffness-dependent cell-matrix interactions. These results underscore the effect of the matrix modulus on the fate of NP-SCs. This research may facilitate elucidation of the complex cross-talk between NP-SCs and their surrounding matrix in healthy as well as pathological conditions. (C) 2015 Elsevier Ltd. All rights reserved.
机译:椎间盘(IVD)变性和随之而来的腰背痛是一项重大的医学挑战。髓核来源的干细胞(NP-SCs)可能导致这种严重疾病的新疗法。最近显示,成熟NP细胞的存活和功能部分受组织硬度的调节。我们假设基质刚度的改变将影响培养的NP-SCs增殖,存活和分化为成熟NP细胞的能力。 NP-SCs在不同硬度的三维矩阵中进行亚培养,通过材料的剪切储能模量进行测量。分析了向成软骨或成骨细胞系的细胞存活,活性和分化速率。 NP-SCs在所有基质中均会增殖和分化,而与基质刚度无关。但是,低剪切储能模量(G'= 1 kPa)的基质促进了更多的增殖和软骨形成分化,而高模量(G'= 2 kPa)的基质则促进了成骨分化。通过共聚焦和扫描电子显微镜进行的成像验证了细胞存活并突出了依赖于硬度的细胞-基质相互作用。这些结果强调了基质模量对NP-SCs命运的影响。这项研究可能有助于阐明在健康以及病理条件下NP-SCs及其周围基质之间的复杂串扰。 (C)2015 Elsevier Ltd.保留所有权利。

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