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Hepatocellular targeted α-tocopherol based pH sensitive galactosylated lipids: design synthesis and transfection studies

机译:基于肝细胞的靶向α-生育酚的pH敏感半乳糖基化脂质:设计合成和转染研究

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摘要

Receptor mediated gene delivery to the liver offers advantages in treating genetic disorders such as hemophilia and hereditary tyrosinemia type I (HTI). Prior findings demonstrated that tethering the d-galactose head group to cationic lipids directs genes to the liver via asialoglycoprotein receptors (ASGPRs). In our continued efforts to develop safer and efficient lipofectins, we demonstrated that cationic lipids bearing α-tocopherol, an antioxidant, as a hydrophobic domain could deliver genes efficiently with high safety profiles in multiple cell lines. Towards developing ASGPR targeted pH sensitive cationic lipids, we have designed a galactosylated cationic lipid (Toc-Gal) with α-tocopherol as the hydrophobic core covalently connected with a pH responsive triazole moiety and a non-targeting control lipid (Toc-OH) without the galactose head group. In this study, we present the design and synthesis of a pH sensitive galactosylated cationic lipid (Toc-Gal), its comparative transfection biology, cellular uptake studies, serum stability and cytotoxicity profiles in both ASGPR positive and negative liver cells, i.e. HepG2 and SK-Hep-1, respectively.
机译:受体介导的向肝脏的基因传递在治疗遗传性疾病(例如血友病和I型遗传性酪氨酸血症)方面具有优势。先前的发现表明,将d-半乳糖头基束缚于阳离子脂质可通过去唾液酸糖蛋白受体(ASGPR)将基因导入肝脏。在我们不断努力开发更安全,更有效的lipofectins的过程中,我们证明了带有α-生育酚(一种抗氧化剂)作为疏水域的阳离子脂质可以在多个细胞系中高效传递具有高安全性特征的基因。为了开发针对ASGPR的pH敏感型阳离子脂质,我们设计了半乳糖基化阳离子脂质(Toc-Gal),其中α-生育酚为疏水性核心,与pH响应三唑部分共价连接,而非目标对照脂质(Toc-OH)不含半乳糖头基。在这项研究中,我们介绍了pH敏感的半乳糖基化阳离子脂质(Toc-Gal)的设计和合成,其比较转染生物学,细胞摄取研究,在ASGPR阳性和阴性肝细胞(即HepG2和SK)中的血清稳定性和细胞毒性谱-Hep-1,分别。

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