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首页> 美国卫生研究院文献>International Journal of Nanomedicine >A novel application of maleimide for advanced drug delivery: in vitro and in vivo evaluation of maleimide-modified pH-sensitive liposomes
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A novel application of maleimide for advanced drug delivery: in vitro and in vivo evaluation of maleimide-modified pH-sensitive liposomes

机译:马来酰亚胺在高级药物递送中的新应用:马来酰亚胺修饰的pH敏感脂质体的体外和体内评价

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Maleimide is a stable and easy-to-handle moiety that rapidly and covalently conjugates thiol groups of cysteine residues in proteins or peptides. Herein, we use maleimide to modify the surface of liposomes in order to obtain an advanced drug delivery system. Employing a small amount (0.3 mol%) of maleimide-polyethylene glycol (PEG) to modify the surface of the liposomes M-GGLG-liposomes, composed of 1,5-dihexadecyl N,N-diglutamyl-lysyl-L-glutamate (GGLG)/cholesterol/poly(ethylene glycol) 1,2-distearoyl-sn-glycero-3-phosphoethanolamine (PEG5000-DSPE)/maleimide-PEG5000-Glu2C18 at a molar ratio of 5:5:0.03:0.03, drug delivery efficiency was remarkably improved both in vitro and in vivo compared to unmodified liposomes (GGLG-liposomes, composed of GGLG/cholesterol/PEG5000-DSPE/PEG5000-Glu2C18 at a molar ratio of 5:5:0.03:0.03). Moreover, this modification did not elicit any detectable increase in cytotoxicity. The maleimide-modification did not alter the physical characteristics of the liposomes such as size, zeta potential, pH sensitivity, dispersibility and drug encapsulation efficiency. However, M-GGLG-liposomes were more rapidly (≥2-fold) internalized into HeLa, HCC1954, and MDA-MB-468 cells compared to GGLG-liposomes. In vivo, M-GGLG-liposomes encapsulating doxorubicin (M-GGLG-DOX-liposomes) also showed a more potent antitumor effect than GGLG-DOX-liposomes and the widely used 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC)-DOX-liposomes after two subcutaneous injections around breast cancer tissue in mice. The biodistribution of liposomes in this model was observed using an in vivo imaging system, which showed that M-GGLG-liposomes were present for significantly longer at the injection site compared to GGLG-liposomes. The outstanding biological functions of the maleimide-modified liposomes as a novel drug delivery system make them ideally suited to a wide range of applications.
机译:马来酰亚胺是一种稳定且易于操作的部分,可快速共价地缀合蛋白质或肽中半胱氨酸残基的巯基。本文中,我们使用马来酰亚胺来修饰脂质体的表面,以获得先进的药物递送系统。使用少量(0.3 mol%)的马来酰亚胺-聚乙二醇(PEG)修饰脂质体的表面M-GGLG-脂质体,由1,5-二十六烷基N,N-二谷氨酰基-赖氨酰-L-谷氨酸组成)/胆固醇/聚乙二醇1,2-二硬脂酰基-sn-甘油-3-磷酸乙醇胺(PEG5000-DSPE)/马来酰亚胺-PEG5000-Glu2C18,摩尔比为5:5:0.03:0.03,药物递送效率为与未修饰的脂质体(GGLG-脂质体,由GGLG /胆固醇/ PEG5000-DSPE / PEG5000-Glu2C18组成,摩尔比为5:5:0.03:0.03)相比,在体外和体内均具有显着改善。而且,这种修饰没有引起细胞毒性的任何可检测的增加。马来酰亚胺修饰没有改变脂质体的物理特性,例如大小,ζ电势,pH敏感性,分散性和药物包封效率。但是,与GGLG脂质体相比,M-GGLG脂质体更快地(≥2倍)内化到HeLa,HCC1954和MDA-MB-468细胞中。在体内,包裹阿霉素的M-GGLG-脂质体(M-GGLG-DOX-脂质体)也比GGLG-DOX-脂质体和广泛使用的1,2-二棕榈酰基-sn-甘油-3-磷酸胆碱(在小鼠的乳腺癌组织周围两次皮下注射后的DPPC-DOX-脂质体。使用体内成像系统观察了该模型中脂质体的生物分布,这表明与GGLG脂质体相比,M-GGLG脂质体在注射部位的存在时间更长。马来酰亚胺修饰的脂质体作为一种新型的药物输送系统,其出色的生物学功能使其非常适合各种应用。

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