首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >A novel small Odorranalectin-bearing cubosomes: Preparation, brain delivery and pharmacodynamic study on amyloid-β 25-35-treated rats following intranasal administration
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A novel small Odorranalectin-bearing cubosomes: Preparation, brain delivery and pharmacodynamic study on amyloid-β 25-35-treated rats following intranasal administration

机译:一种新型的带有小去甲肾上腺素的小立方体:鼻内给药后对β-淀粉样蛋白25-35治疗的大鼠的制备,脑传递和药效学研究

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摘要

Because of the immunogenicity and toxicity in vivo of large molecules such as lectins, the application of these molecules is remarkably restricted in drug delivery systems. In this study, to improve the brain drug delivery and reduce the immunogenicity of traditional lectin modified delivery system, Odorranalectin (OL, 1700 Da), a novel non-immunogenic small peptide, was selected to establish an OL-modified cubosomes (Cubs) system. The streptavidin (SA)-conjugated Cubs were prepared by incorporating maleimide-PEG-oleate and taking advantage of its thiol group binding reactivity to conjugate with 2-iminothiolane thiolated SA; mono-biotinylated OL was then coupled with the SA-modified Cubs. The OL-decorated Cubs (OL-Cubs) devised via a non-covalent SA-biotin "bridge" made it easy to conjugate OL and determine the number of ligands on the surface of the Cubs using sensitive chemiluminescent detection. Retention of the bio-recognitive activity of OL after covalent coupling was verified by hemagglutination testing. Nose-to-brain delivery characteristic of OL-Cubs was investigated by in vivo fluorescent biodistribution using coumarin-6 as a marker. The relative uptake of coumarin carried by OL-Cubs was 1.66- to 3.46-fold in brain tissues compared to that incorporated in the Cubs. Besides, Gly14-Humanin (S14G-HN) as a model peptide drug was loaded into cubosomes and evaluated for its pharmacodynamics on Alzheimer's disease (AD) rats following intranasal administration by Morris water maze test and acetylcholinesterase activity determination. The results suggested that OL functionalization enhanced the therapeutic effects of S14G-HN-loaded cubosomes on AD. Thus, OL-Cubs might offer a novel effective and noninvasive system for brain drug delivery, especially for peptides and proteins.
机译:由于大分子例如凝集素的体内免疫原性和毒性,这些分子的应用在药物递送系统中受到显着限制。在这项研究中,为改善脑部药物的输送并降低传统凝集素修饰的传递系统的免疫原性,选择了一种新型的非免疫原性小肽Odorranalectin(OL,1700 Da)建立了OL修饰的立方体(Cubs)系统。 。通过掺入马来酰亚胺-PEG-油酸酯并利用其硫醇基团与2-亚氨基硫杂环戊烷硫醇化SA结合的结合反应性来制备链霉亲和素(SA)结合的Cub。然后将单生物素化的OL与SA修饰的Cub偶联。通过非共价SA-生物素“桥”设计的OL装饰小熊(OL-Cubs)使结合OL变得容易,并使用灵敏的化学发光检测确定了小熊表面上的配体数量。通过血凝试验验证了共价偶联后OL的生物识别活性的保留。通过使用香豆素6作为标记的体内荧光生物分布研究了OL-Cub的从鼻到脑的输送特性。 OL-Cub携带的香豆素在大脑组织中的相对摄取量是Cubs摄取的相对摄取量的1.66-3.46倍。此外,通过莫里斯水迷宫试验和乙酰胆碱酯酶活性测定,鼻内给药后,将作为模型肽药物的Gly14-Humanin(S14G-HN)装入立方脂质体,并评估其对阿尔茨海默氏病(AD)大鼠的药效。结果表明,OL功能化可增强S14G-HN负载的立方脂质体对AD的治疗效果。因此,OL-Cubs可能为脑部药物输送,尤其是肽和蛋白质的输送,提供一种新颖有效的无创系统。

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