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Development of a peptide-targeted, myocardial ischemia-homing, mesenchymal stem cell

机译:靶向肽,心肌缺血归巢,间充质干细胞的开发

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Directing stem cells to the heart is critical in producing an effective cell therapy for myocardial infarction (MI). Mesenchymal stem cells (MSCs) offer an exquisite drug delivery platform with environment-sensing cytokine release and MSCs have shown therapeutic potential in MI. Peptide-based targeting offers a novel method to increase cell homing, wherein MI-specific peptides, identified by phage display, are synthesized with a palmitic acid tail to facilitate cell membrane integration. Phage-peptides were screened in a mouse MI model and four peptides (CRPPR, CRKDKC, KSTRKS, and CARSKNKDC) were selected and synthesized as palmitated derivatives for further investigation. Cell coating was optimized and coating persistence and cytotoxicity were evaluated. MSCs were coated with peptides, injected into mice with MI, and MSCs in the heart quantified. Greater numbers of MSCs were found in heart of animals treated with the peptide-coated MSCs compared to uncoated controls. MSC numbers had positive correlation with MI severity in peptide-coated cells but a negative correlation in MSCs alone. A transient cell coating ("painting") method has been developed that labels cells efficiently, non-toxically and increases cell localization in MI hearts.
机译:将干细胞引导至心脏对于产生有效的心肌梗塞(MI)细胞疗法至关重要。间充质干细胞(MSC)提供了具有环境敏感型细胞因子释放的精美药物递送平台,并且MSC已显示出对MI的治疗潜力。基于肽的靶向提供了增加细胞归巢的新方法,其中通过噬菌体展示鉴定的MI特异性肽与棕榈酸尾部合成,以促进细胞膜整合。在小鼠MI模型中筛选了噬菌体肽,并选择了4种肽(CRPPR,CRKDKC,KSTRKS和CARSKNKDC)并合成为棕榈酸酯化的衍生物,以供进一步研究。优化细胞涂层并评估涂层的持久性和细胞毒性。用肽包被MSC,将其注射入MI小鼠体内,并对心脏中的MSC进行定量。与未包被的对照相比,在用肽包被的MSC处理的动物心脏中发现了更多的MSC。 MSC数目与包被肽细胞的MI严重程度呈正相关,而仅在MSC中呈负相关。已经开发出一种瞬时细胞包被(“涂漆”)方法,该方法可以有效,无毒地标记细胞并增加MI心脏的细胞定位。

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