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Polysaccharide Hydrogels Support the Long-Term Viability of Encapsulated Human Mesenchymal Stem Cells and Their Ability to Secrete Immunomodulatory Factors

机译:多糖水凝胶支持包封的人间充质干细胞的长期活力及其分泌免疫调节因子的能力

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While therapeutically interesting, the injection of MSCs suffers major limitations including cell death upon injection and a massive leakage outside the injection site. We proposed to entrap MSCs within spherical particles derived from alginate, as a control, or from silanized hydroxypropyl methylcellulose (Si-HPMC). We developed water in an oil dispersion method to produce small Si-HPMC particles with an average size of about 68?μm. We evidenced a faster diffusion of fluorescein isothiocyanate-dextran in Si-HPMC particles than in alginate ones. Human adipose-derived MSCs (hASC) were encapsulated either in alginate or in Si-HPMC, and the cellularized particles were cultured for up to 1 month. Both alginate and Si-HPMC particles supported cell survival, and the average number of encapsulated hASC per alginate and Si-HPMC particle (7102 and 5100, resp.) did not significantly change. The stimulation of encapsulated hASC with proinflammatory cytokines resulted in the production of IDO, PGE2, and HGF whose concentration was always higher when cells were encapsulated in Si-HPMC particles than in alginate ones. We have demonstrated that Si-HPMC and alginate particles support hASC viability and the maintenance of their ability to secrete therapeutic factors.
机译:在治疗上有趣的同时,注射MSCs在注射时遭受细胞死亡的主要限制,并且在注射部位外漏气。我们提出诱捕来自藻酸盐的球形颗粒内的MSC,作为对照,或来自硅烷化羟丙基甲基纤维素(Si-HPMC)。我们在油分散方法中开发了水,生产小的Si-HPMC颗粒,平均尺寸为约68Ωμm。我们在Si-HPMC颗粒中证明了荧光素异硫氰酸酯 - 葡聚糖的扩散速度而不是藻酸盐颗粒。人的脂肪衍生的MSCs(HASC)包封在藻酸盐中或在Si-HPMC中包封,并且细胞化颗粒培养至1个月。藻酸盐和Si-HPMC颗粒都支持细胞存活,并且每藻酸盐和Si-HPMC颗粒的平均包封的HASc(7102和5100,REAC。)没有显着改变。用促炎细胞的包封的HASC的刺激导致MAO,PGE2和HGF的产生,当细胞包封在Si-HPMC颗粒中的浓度总是较高的,而不是在藻酸盐颗粒中。我们已经证明,Si-HPMC和海藻酸盐颗粒支持HASC存活率和维持其分泌治疗因素的能力。

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