首页> 外文期刊>Bulletin of the Korean Chemical Society >Comparison of Drug Delivery Efficiency between Doxorubicin Intercalated in RNA Aptamer and One Encapsulated in RNA Aptamer-Conjugated Liposome
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Comparison of Drug Delivery Efficiency between Doxorubicin Intercalated in RNA Aptamer and One Encapsulated in RNA Aptamer-Conjugated Liposome

机译:插入在RNA适体中的阿霉素与包裹在RNA适体缀合的脂质体中的一种阿霉素之间的药物传递效率比较

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摘要

Combination of drug delivery and specific targeting has the potential for treating cancers. To achieve this goal, specific ligands targeting cancer cells and bioconjugate vehicles for drug delivery are necessary. Liposomes constitute successful drug-delivery materials because they can reduce toxicity and enhance the stability of drugs by encapsulation. Previously, we have developed an RNA aptamer-conjugated liposome (named as aptamosome) that specifically targeted prostate cancer cells expressing prostate-specific membrane antigen (PSMA). Using the aptamosome, the anticancer drug doxorubicin (Dox) was specifically and efficiently delivered to the prostate tumors. The PSMA-specific RNA aptamer by itself has been also recognized as tumor-specific drug delivery material by intercalating Dox. In this study, we compared two different methods for Dox delivery toward PSMA-positive cancer cells, namely intercalation of Dox into the aptamer (Apt-Dox), and encapsulation of Dox in the aptamosome (Apm-Dox). We observed that the Apm-Dox was superior to the Apt-Dox in specificity and Dox delivery efficiency toward PSMA(+) cancer cells.
机译:药物递送和特异性靶向的组合具有治疗癌症的潜力。为了实现该目标,需要靶向癌细胞的特异性配体和用于药物递送的生物缀合物载体。脂质体构成成功的药物递送材料,因为它们可以通过封装降低毒性并增强药物的稳定性。以前,我们已经开发了RNA适体偶联脂质体(称为aptamosome),该脂质体专门靶向表达前列腺特异性膜抗原(PSMA)的前列腺癌细胞。使用适体将抗癌药阿霉素(Dox)特异性有效地递送至前列腺肿瘤。通过插入Dox,PSMA特异性RNA适体本身也被认为是肿瘤特异性药物递送材料。在这项研究中,我们比较了将Dox传递到PSMA阳性癌细胞的两种不同方法,即将Dox插入适体(Apt-Dox)和将Dox封装在适体中(Apm-Dox)。我们观察到,Apm-Dox在针对PSMA(+)癌细胞的特异性和Dox输送效率方面优于Apt-Dox。

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