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Effect of cationic lipid in cationic liposomes on siRNA delivery into the lung by intravenous injection of cationic lipoplex

机译:阳离子脂质脂质脂质脂质对静脉注射阳离子剂量静脉注射液体脂质脂质体的影响

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Cationic liposomes composed of dialkyl cationic lipid such as 1,2-dioleoyl-3-trimethylammonium-propane (DOTAP) can efficiently deliver siRNA to the lungs following the intravenous injection of cationic lipo-some/siRNA complexes (lipoplexes). In this study, we examined the effect of cationic lipid of cationic liposomes on siRNA delivery to the lungs after intravenous injection. We used six kinds of cationic cholesterol derivatives and 11 kinds of dialkyl or trialkyl cationic lipids as cationic lipids, and prepared 17 kinds of cationic liposomes composed of a cationic lipid and 1,2-dioleoyl-L-alpha-glycero-3-phosphatidylethanolamine (DOPE) for evaluation of siRNA biodistribution and in vivo gene silencing effects. Among cationic liposomes, those composed of N-hexadecyl-N,N-dimethylhexadecan-1-aminium bromide (DC-1-16), N,N-dimethyl-N-octadecyloctadecan-1-aminium bromide (DC-1-18), 2-((1,5-bis(octadecyloxy)-1,5-dioxopen-tan-2-yl)amino)-N,N,N-trimethyl-2-oxoethan-1-aminium chloride (DC-3-18D), 11-((1,3-bis(dodecanoyloxy)-2-((dodecanoyloxy)methyl)propan-2-yl)amino)-N,N,N-trimethyl-11-oxoundecan-1-aminium bromide (TC-1-12), or cholesteryl (3-((2-hydroxyethyl)amino)propyl)carbamate hydroiodide (HAPC-Chol) with DOPE exhibited high accumulation of siRNA in the lung and significant suppression of Tie2 mRNA expression after the intravenous injection of cationic lipoplexes with Tie2 siRNA. Furthermore, DC-1-16/DOPE and DC-1-18/ DOPE lipoplexes with protein kinase N3 (PKN3) siRNA could suppress the tumour growth when intravenously injected into mice with lung LLC metastasis. These findings indicate that the siRNA biodistribution and in vivo knockdown efficiency after the intravenous injection of cationic lipoplexes were strongly affected by the type of cationic lipid of cationic liposomes.
机译:由二烷基阳离子脂质组成的阳离子脂质体如1,2-二脲-3-三甲基丙烷 - 丙烷(DOTAP)可以在静脉内注射阳离子脂质 - 一些/ siRNA复合物(脂质物)后有效地将siRNA递送至肺部。在这项研究中,我们检查了静脉注射后阳离子脂质体阳离子脂质体对肺部肺的影响。我们使用六种阳离子胆固醇衍生物和11种二烷基或三烷基阳离子脂质作为阳离子脂质,并制备的17种阳离子脂质体组成,由阳离子脂质和1,2-二脲-1-α-甘油-3-磷脂酰乙醇胺(掺杂剂,用于评估siRNA生物分布和体内基因沉默效果。在阳离子脂质体中,由N-十六烷基-N,N-二甲基己二烷烷-1-溴化铵(DC-1-16),N,N-二甲基-N-十八烷基苯基烷-1-氨基溴化物(DC-1-18)组成的那些。 ,2 - ((1,5-双(十八烷基氧氧基)-1,5-二恶烷酸甲酯-2-基-2-基)氨基)-N,N,N-三甲基-2-氧代苯乙烷-1-氨基氯(DC-3- 18d),11 - ((1,3-双(十二烷酰氧基)-2 - ((十二烷酰氧基)甲基)丙烷-2-基)氨基)-N,N,N-三甲基-11-羟基癸酸-1-氨基溴( TC-1-12),或胆固醇(3-((2-羟基乙基)氨基)丙基)氨基甲酸酯氢碘酰胺(HAPC-CHOL)具有掺杂的肺部含量高,静脉注射后的TiE2 mRNA表达的显着抑制阳离子脂肪量与Tie2 siRNA。此外,DC-1-16 /掺杂剂和DC-1-18 /掺杂剂脂肪量与蛋白激酶N3(PKN3)siRNA可以在用肺部LLC转移静脉内注射到小鼠中时抑制肿瘤生长。这些发现表明siRNA生物分布和体内敲低效率后,静脉注射阳离子脂质物质后受到阳离子脂质脂质的脂质的影响。

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