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海藻酸钠微球控释大鼠脂肪干细胞。

Controlled release of rat adipose-derived stem cells from alginate microbeads.

机构信息

Wallace H. Coulter Department of Biomedical Engineering at Georgia Tech and Emory University, Georgia Institute of Technology, Atlanta, GA, USA.

出版信息

Biomaterials. 2013 Nov;34(33):8172-84. doi: 10.1016/j.biomaterials.2013.07.017. Epub 2013 Jul 29.

Abstract

Cell-based therapies have potential for tissue regeneration but poor delivery methods lead to low viability or dispersal of cells from target sites, limiting clinical utility. Here, we developed a degradable and injectable hydrogel to deliver stem cells for bone regeneration. Alginate microbeads <200 μm are injectable, persist at implantation sites and contain viable cells, but do not readily degrade in-vivo. We hypothesized that controlled release of rat adipose-derived stem cells (ASCs) from alginate microbeads can be achieved by incorporating alginate-lyase in the hydrogel. Microbeads were formed using high electrostatic potential. Controlled degradation was achieved through direct combination of alginate-lyase and alginate at 4 °C. Results showed that microbead degradation and cell release depended on the alginate-lyase to alginate ratio. Viability of released cells ranged from 87% on day 2 to 71% on day 12. Monolayer cultures of released ASCs grown in osteogenic medium produced higher levels of osteocalcin and similar levels of other soluble factors as ASCs that were neither previously encapsulated nor exposed to alginate-lyase. Bmp2, Fgf2, and Vegfa mRNA in released cells were also increased. Thus, this delivery system allows for controlled release of viable cells and can modulate their downstream osteogenic factor production.

摘要

基于细胞的疗法具有组织再生的潜力,但较差的输送方法导致细胞的存活率低或从靶部位分散,限制了临床应用。在这里,我们开发了一种可降解和可注射的水凝胶,用于输送干细胞进行骨再生。小于 200μm 的海藻酸盐微球可注射,在植入部位保持存在并含有存活的细胞,但在体内不易降解。我们假设通过在水凝胶中加入海藻酸盐裂解酶,可以实现从海藻酸盐微球中释放大鼠脂肪来源干细胞(ASCs)的控制释放。微球是使用高静电势形成的。通过在 4°C 下直接组合海藻酸盐裂解酶和海藻酸盐,实现了可控降解。结果表明,微球的降解和细胞的释放依赖于海藻酸盐裂解酶与海藻酸盐的比例。释放细胞的活力从第 2 天的 87%到第 12 天的 71%不等。在成骨培养基中生长的释放 ASC 的单层培养物产生的骨钙素水平更高,而其他可溶性因子的水平与既未先前包封也未暴露于海藻酸盐裂解酶的 ASC 相似。释放细胞中的 Bmp2、Fgf2 和 Vegfa mRNA 也增加了。因此,该输送系统允许释放有活力的细胞,并可以调节其下游成骨因子的产生。

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