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通过糖蛋白 H 衍生肽偶联的纳米乳液增强药物向细胞胞质溶胶的递送。

Enhanced Drug Delivery into Cell Cytosol via Glycoprotein H-Derived Peptide Conjugated Nanoemulsions.

机构信息

Center for Advanced Biomaterials for Health Care@CRIB, Istituto Italiano di Tecnologia , Largo Barsanti e Matteucci 53, Napoli 80125, Italy.

Interdisciplinary Research Center of Biomaterials, CRIB, University Federico II , P.le Tecchio 80, Naples 80125, Italy.

出版信息

ACS Nano. 2017 Oct 24;11(10):9802-9813. doi: 10.1021/acsnano.7b03058. Epub 2017 Aug 28.

DOI:10.1021/acsnano.7b03058
PMID:28820568
Abstract

The key role of nanocarriers in improving the pharmacological properties of commonly used drugs is recognized worldwide. It is also known that in the development of new effective nanocarriers the use of targeting moieties integrated on their surface is essential. Herein, we propose a nanocarrier based on an oil in water nanoemulsion coated with a membranotropic peptide derived from the glycoprotein H of Herpes simplex virus 1, known as gH625, in order to reduce endolysosomal accumulation and to enhance cytosolic localization. In addition, we show an enhanced anti-inflammatory activity of curcumin, a bioactive compound isolated from the Curcuma longa plant, when loaded into our engineered nanocarriers. This effect is a consequence of a higher uptake combined with a high curcumin preservation exerted by the active nanocapsules compared to control ones. When loaded into our nanocapsules, indeed, curcumin molecules are directly internalized into the cytosol rather than into lysosomes. Further, in order to extend the in vitro experimental setting with a more complex model and to explore the possibility to use our nanocarriers for further biological applications, we tested their performance in a 3D sprouting angiogenesis model. Finally, we show promising preliminary in vivo results by assessing the anti-inflammatory properties of the proposed nanocarrier.

摘要

纳米载体在改善常用药物的药理学性质方面起着关键作用,这在全球范围内得到认可。人们还知道,在开发新的有效纳米载体时,必须在其表面整合靶向部分。在此,我们提出了一种基于油包水纳米乳液的纳米载体,该纳米乳液由单纯疱疹病毒 1 的糖蛋白 H 衍生的膜转位肽(称为 gH625)包被,以减少内溶酶体积累并增强细胞溶质定位。此外,我们还展示了姜黄素(一种从姜黄植物中分离出的生物活性化合物)在负载到我们设计的纳米载体中时具有增强的抗炎活性。这种效果是由于与对照相比,活性纳米胶囊具有更高的摄取率和更高的姜黄素保留率。实际上,当负载到我们的纳米胶囊中时,姜黄素分子直接被内吞到细胞质中,而不是溶酶体中。此外,为了将体外实验设置扩展到更复杂的模型,并探索将我们的纳米载体用于进一步生物学应用的可能性,我们在 3D 发芽血管生成模型中测试了它们的性能。最后,通过评估所提出的纳米载体的抗炎特性,我们展示了有希望的初步体内结果。

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