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The development of EH networks for skeletal muscle regeneration within abdominal wall hernias.

机译:EH网络在腹壁疝内骨骼肌再生的发展。

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Incisional hernias are a common clinical problem occurring in up to 10% of all patients undergoing abdominal incisions. Current repair techniques involve the placement of xenografts, allografts, or prosthetic biomaterials. Despite these techniques, the incidence of hernia recurrence ranges from 24% to 54%. In order to address these high recurrence rates, we propose using a skeletal muscle engineering strategy. To this end, the novel cyclic acetal biomaterial, 5-ethyl-5-(hydroxymethyl)-beta,beta-dimethyl-1,3-dioxane-2-ethanol diacrylate, was functionalized to promote skeletal muscle regeneration. It was found that this biomaterial promotes myoblastic cell attachment and proliferation as well as the delivery of functional insulin-like growth factor 1 proteins in vitro; therefore demonstrating the scaffolds biocompatibility. Furthermore, mechanical properties of the scaffold were tested and the complex modulus was shown to decrease after a significant increase in initiator concentration. Overall, this work establishes the functionality of a degradable cyclic acetal as a scaffold for skeletal muscle engineering.
机译:切口疝是常见的临床问题,在所有接受腹部切口的患者中,多达10%发生。当前的修复技术涉及异种移植物,同种异体移植物或人工生物材料的放置。尽管有这些技术,疝气复发的发生率范围为24%至54%。为了解决这些高复发率,我们建议使用骨骼肌工程学策略。为此,将新型环状缩醛生物材料5-乙基-5-(羟甲基)-β,β-二甲基-1,3-二恶烷-2-乙醇二丙烯酸酯官能化以促进骨骼肌再生。已经发现,这种生物材料在体外促进成肌细胞附着和增殖以及功能性胰岛素样生长因子1蛋白的递送。因此证明了支架的生物相容性。此外,测试了支架的机械性能,并显示出引发剂浓度显着增加后,复数模量降低。总的来说,这项工作建立了可降解的环状缩醛作为骨骼肌工程支架的功能。

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