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Biofabrication of a novel leukocyte‐fibrin‐platelet membrane as a cells and growth factors delivery platform for tissue engineering applications

机译:生物结缔组新型白细胞纤维蛋白 - 血小板膜作为组织工程应用的细胞和生长因子输送平台

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Abstract Autologous platelet‐rich hemocomponents have emerged as potential biologic tools for regenerative purpose, but their therapeutic efficacy still remains controversial. This work represents the characterization study of an innovative autologous leukocyte‐fibrin‐platelet membrane (LFPm), which we prepared according to a novel protocol involving multiple cycles of apheresis. The high content in fibrinogen gave to our hemocomponent the appearance of a manipulable and suturable membrane with high elasticity and deformation capacity. Moreover, being highly enriched with platelets, leukocytes, and monocytes/macrophages, the LFPm sustained the local release of bioactive molecules (platelet derived growth factor, vascular endothelial growth factor, interleukin‐10, and tumour necrosis factor alpha). In parallel, the evaluation of stemness potential highlighted also that the LFPm contained cells expressing pluripotency and multipotency markers both at the messenger ribonucleic acid ( NANOG , SOX2 , THY1 , NT5E , and ENG ) and surface‐protein level (CD44 high /CD73 + /CD34 + /CD117 + /CD31 + ). Finally, biodegradation analysis interestingly showed a good stability of the membrane for at least 3?weeks in vitro and 1?week in vivo. In both cases, biodegradation was associated with progressive exposure of fibrin scaffold, loss/migration of cellular elements, and release of growth factors. Overall, collected evidence could shed some light on the regenerative effect that LFPms may exert after the autologous implant on a defect site.
机译:摘要自体血小板血液中的血液组成是潜在的再生目的的潜在生物学工具,但它们的治疗效果仍然存在争议。这项工作代表了一种创新的自体白细胞 - 纤维蛋白 - 血浆膜(LFPM)的表征研究,我们根据涉及多个循环的吸腹循环的新方案制备。纤维蛋白原中的高含量为我们的血液组成具有高弹性和变形能力的可操纵和耐润膜的外观。此外,高度富含血小板,白细胞和单核细胞/巨噬细胞,LFPM持续了生物活性分子的局部释放(血小板衍生的生长因子,血管内皮生长因子,白细胞介素-10和肿瘤坏死因子α)。并行地,茎孔潜能的评估还突出显示,在信使核糖核酸(纳米,SOX2,THY1,NT5E和ENG)和表面蛋白质水平(CD44高/ CD73 + / / CD34 + / CD117 + / CD31 +)。最后,有趣的生物降解分析有趣地显示出膜的良好稳定性至少3°(体外)体外和1周内。在这两种情况下,生物降解与纤维蛋白支架,损失/迁移细胞元素的渐进暴露,以及释放生长因子。总体而言,收集的证据可以在缺陷部位上的自体植入后可能发出的再生效果,从而阐明了一些光。

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