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首页> 外文期刊>Journal of biomaterials applications >Injectable, redox-polymerized carboxymethylcellulose hydrogels promote nucleus pulposus-like extracellular matrix elaboration by human MSCs in a cell density-dependent manner
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Injectable, redox-polymerized carboxymethylcellulose hydrogels promote nucleus pulposus-like extracellular matrix elaboration by human MSCs in a cell density-dependent manner

机译:可注射的氧化还原聚合的羧甲基纤维素水凝胶促进人体MSCs以细胞密度依赖性方式促进核浆状的细胞外基质阐述

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摘要

Low back pain is a major cause for disability and is closely linked to intervertebral disc degeneration. Mechanical and biological dysfunction of the nucleus pulposus in the disc has been found to initiate intradiscal degenerative processes. Replacing or enriching the diseased nucleus pulposus with an injectable, stem cell-laden biomaterial that mimics its material properties can provide a minimally invasive strategy for biological and structural repair of the tissue. In this study, injectable, in situ-gelling carboxymethylcellulose hydrogels were developed for nucleus pulposus tissue engineering using encapsulated human marrow-derived mesenchymal stromal cells (hMSCs). With the goal of obtaining robust extracellular matrix deposition and faster construct maturation, two cell-seeding densities, 20x10(6) cells/ml and 40x10(6) cells/ml, were examined. The constructs were fabricated using a redox initiation system to yield covalently crosslinked, cell-seeded hydrogels via radical polymerization. Chondrogenic culture of the hydrogels over 35 days exhibited high cell viability along with deposition of proteoglycan and collagen-rich extracellular matrix, and mechanical and swelling properties similar to native human nucleus pulposus. Further, the matrix production and distribution in the carboxymethylcellulose hydrogels was found to be strongly influenced by hMSC-seeding density, with the lower cell-seeding density yielding a more favorable nucleus pulposus-specific matrix phenotype, while the rate of construct maturation was less dependent on the cell-seeding density. These findings are the first to demonstrate the utility of redox-polymerized carboxymethylcellulose hydrogels as hMSC carriers for potential minimally invasive treatment strategies for nucleus pulposus replacement.
机译:低腰疼痛是残疾的主要原因,与椎间盘变性密切相关。已经发现盘中核浆气的机械和生物功能障碍引发脑内退行性方法。用可注射的干细胞含水剂替代或富含患病的核浆料,其模拟其材料特性可以为组织的生物和结构修复提供微创策略。在该研究中,用于使用包封的人骨髓衍生的间充质细胞(HMSCs)的核浆组织工程开发出原位胶凝羧甲基纤维素水凝胶。通过获得稳健的细胞外基质沉积和更快的构建成熟,检查两个细胞播种密度,20×10(6)个细胞/ mL和40×10(6)细胞/ mL。使用氧化还原引发系统制造构建体,得到通过自由基聚合产生共价交联的细胞接种水凝胶。水凝胶的软骨培养物超过35天表现出高细胞活力,以及致蛋白质酚和富含胶原蛋白的细胞外基质的沉积,以及类似于天然人核瓜素的机械和溶胀性能。此外,发现羧甲基纤维素水凝胶中的基质产生和分布受HMSC播种密度的强烈影响,较低的细胞播种密度产生更有利的细胞核牙髓特异性基质表型,而构建成熟率较小关于细胞播种密度。这些发现是首先证明氧化还原聚合的羧甲基纤维素水凝胶作为HMSC载体的效用,用于核心髓鞘替代的潜在侵入性治疗策略。

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