首页> 美国卫生研究院文献>ACS AuthorChoice >Cell Therapy with Embryonic Stem Cell-Derived Cardiomyocytes Encapsulated in Injectable Nanomatrix Gel Enhances Cell Engraftment and Promotes Cardiac Repair
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Cell Therapy with Embryonic Stem Cell-Derived Cardiomyocytes Encapsulated in Injectable Nanomatrix Gel Enhances Cell Engraftment and Promotes Cardiac Repair

机译:封装在可注射纳米基质凝胶中的胚胎干细胞衍生的心肌细胞的细胞疗法增强细胞植入并促进心脏修复。

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摘要

A significant barrier to the therapeutic use of stem cells is poor cell retention in vivo. Here, we evaluate the therapeutic potential and long-term engraftment of cardiomyocytes (CMs) derived from mouse embryonic stem cells (mESCs) encapsulated in an injectable nanomatrix gel consisting of peptide amphiphiles incorporating cell adhesive ligand Arg-Gly-Asp-Ser (PA-RGDS) in experimental myocardial infarction (MI). We cultured rat neonatal CMs in PA-RGDS for 7 days and found that more than 90% of the CMs survived. Next, we intramyocardially injected mouse CM cell line HL-1 CMs with or without PA-RGDS into uninjured hearts. Histologic examination and flow cytometry analysis of digested heart tissues showed approximately 3-fold higher engraftment in the mice that received CMs with PA-RGDS compared to those without PA-RGDS. We further investigated the therapeutic effects and long-term engraftment of mESC-CMs with PA-RGDS on MI in comparison with PBS control, CM-only, and PA-RGDS only. Echocardiography demonstrated that the CM-only and CM+PA-RGDS groups showed higher cardiac function at week 2 compared to other groups. However, from 3 weeks, higher cardiac function was maintained only in the CM+PA-RGDS group; this was sustained for 12 weeks. Confocal microscopic examination of the cardiac tissues harvested at 14 weeks demonstrated sustained engraftment and integration of mESC-CMs into host myocardium in the CM+PA-RGDS group only. This study for the first time demonstrated that PA-RGDS encapsulation can enhance survival of mESC-derived CMs and improve cardiac function post-MI. This nanomatrix gel-mediated stem cell therapy can be a promising option for treating MI.
机译:干细胞治疗用途的重要障碍是体内不良细胞滞留。在这里,我们评估了源自小鼠胚胎干细胞(mESCs)的心肌细胞(CMs)的治疗潜力和长期移植性,该小鼠胚胎干细胞(mESCs)封装在可注射的纳米基质凝胶中,该凝胶由掺有细胞粘附配体Arg-Gly-Asp-Ser(PA- RGDS)在实验性心肌梗死(MI)中。我们在PA-RGDS中培养了7天的大鼠新生CM,发现90%以上的CM幸存下来。接下来,我们将心肌内或无PA-RGDS的小鼠CM细胞系HL-1 CMs注入未受伤的心脏。消化的心脏组织的组织学检查和流式细胞术分析表明,与不使用PA-RGDS的小鼠相比,接受了PA-RGDS的CM的小鼠的植入率高约3倍。与PBS对照,仅CM和仅PA-RGDS相比,我们进一步研究了mESC-CM与PA-RGDS对MI的治疗效果和长期植入。超声心动图表明,与其他组相比,仅CM组和CM + PA-RGDS组在第2周显示出更高的心脏功能。但是,从3周开始,仅CM + PA-RGDS组才保持较高的心脏功能。这持续了12周。共聚焦显微镜检查在第14周采集的心脏组织表明,仅在CM + PA-RGDS组中,mESC-CM持续移入并整合到宿主心肌中。这项研究首次证明,PA-RGDS封装可以提高源自mESC的CM的存活率,并改善MI后的心脏功能。这种纳米基质凝胶介导的干细胞疗法可能是治疗MI的有前途的选择。

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