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首页> 外文期刊>Molecular Systems Design & Engineering >Therapeutic peptide delivery via aptamer- displaying, disulfide-linked peptide amphiphile micelles
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Therapeutic peptide delivery via aptamer- displaying, disulfide-linked peptide amphiphile micelles

机译:通过适配子——治疗肽交付显示,disulfide-linked肽两亲物胶束

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摘要

Peptide amphiphile micelles (PAMs) are a powerful platform technology for improving the delivery of therapeutic and prophylactic peptides. While previous research has shown aptamer-displaying PAMs enhance cell association, transportation to intracellular targets still remains a substantial hurdle for these biomaterials. In this article, we detail our efforts to address this challenge through the creation of disulfide- linked peptide amphiphile (PAs). These molecules were found to self-assemble in water into PAMs for which lipidated DNA oligomers ( antitail amphiphiles – AAs) could be entrapped and used to tether aptamers (Apt) to the nanoparticle surface. These Apt~A/PAMs were physically characterized and evaluated for their blood-serum stability using fetal bovine serum exposure and glutathione reduction. To assess their enhanced intracellular delivery capacity and therapeutic functionality, PAMs bearing cell-penetrating peptide modified “Plenty of SH3 domains” scaffold protein competitive inhibitor (Tat-POSH) and B cell lymphoma targeting aptamer (C10.36) were incubated with Ramos cells, a non-Hodgkin lymphoma cell line. C10.36~A/PAMs were found not only to be stable in blood-like conditions, but also to be capable of facilitating delivery of therapeutic Tat-POSH peptide to Ramos cells .
机译:肽两亲物胶束(PAMs)是一个强大的平台技术改善的交付治疗和预防肽。之前的研究表明aptamer-displayingPAMs增强细胞协会、运输细胞内目标仍然很大对这些生物材料的障碍。我们详细地努力应对这一挑战通过创建二硫-肽有关亲水脂分子(PAs)。在水中自组装成PAMs的原子吸收光谱法)可以裹入和使用范围寡核苷酸适配子(Apt)纳米粒子表面。恰当的~ / PAMs身体特征,评估他们的血清稳定使用胎牛血清暴露,谷胱甘肽减少。交付能力和治疗功能,PAMs轴承cell-penetrating肽修改“很多SH3域”脚手架蛋白竞争性抑制剂(Tat-POSH)和B细胞淋巴瘤针对适配子(C10.36)非霍奇金孵化与拉莫斯细胞淋巴瘤细胞株。只有在作品中条件是稳定的,但是还能促进交付治疗Tat-POSH肽拉莫斯细胞。

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