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Multifunctional cationic nanosystems for nucleic acid therapy of thoracic aortic dissection

机译:胸主动脉夹层核酸治疗多功能阳离子纳米系统

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Thoracic aortic dissection (TAD) is an aggressive vascular disease that requires early diagnosis and effective treatment. However, due to the particular vascular structure and narrowness of lesion location, there are no effective drug delivery systems for the therapy of TAD. Here, we report a multifunctional delivery nanosystem (TP-Gd/miRNA-ColIV) composed of gadolinium-chelated tannic acid (TA), low-toxic cationic PGEA (ethanolamine-aminated poly(glycidyl methacrylate)) and type IV collagen targeted peptide (ColIV) for targeted nucleic acid therapy, early diagnosis and noninvasive monitoring of TAD. Such targeted therapy with miR-145 exhibits impressive performances in stabilizing the vascular structures and preventing the deterioration of TAD. After the treatment with TP-Gd/miR-145-ColIV, nearly no dissection occurs in the thoracic aortic arches of the mice with TAD model. Moreover, TP-Gd/miRNA-ColIV also demonstrates good magnetic resonance imaging (MRI) ability and can be used to noninvasively monitor the development conditions of TAD.
机译:胸主动脉夹层(TAD)是一种腐蚀性的血管疾病,需要早期诊断和有效治疗。然而,由于特定的血管结构和病变位置的窄性,没有有效的药物递送系统用于TAD的治疗。在这里,我们报告了由钆螯合鞣酸(TA),低毒阳离子PGEA(乙醇胺酰胺聚(甲基丙烯酸酯))和IV型胶原蛋白靶向肽( COLIV)用于靶向核酸治疗,早期诊断和TAD的非侵入性监测。 MiR-145的这种靶向治疗表现出令人印象深刻的性能,稳定血管结构并防止TAD的恶化。在用TP-GD / miR-145-COIV治疗后,在具有TAD模型的小鼠的胸主动脉拱门中几乎没有剖析。此外,TP-GD / MIRNA-COIV还证明了良好的磁共振成像(MRI)能力,可用于非侵入地监测TAD的发育条件。

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