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壳聚糖 - N - 乙酰半胱氨酸包被香豆素 - 6标记的纳米结构脂质载体对兔眼内分布影响的体外和体内评价

Ex Vivo and in Vivo Evaluation of the Effect of Coating a Coumarin-6-Labeled Nanostructured Lipid Carrier with Chitosan-N-acetylcysteine on Rabbit Ocular Distribution.

作者信息

Liu Dandan, Li Jinyu, Cheng Bingchao, Wu Qingyin, Pan Hao

机构信息

School of Biomedical & Chemical Engineering, Liaoning Institute of Science and Technology , Benxi 117004, P. R. China.

School of Pharmacy, Shenyang Pharmaceutical University , Shenyang 110016, P. R. China.

出版信息

Mol Pharm. 2017 Aug 7;14(8):2639-2648. doi: 10.1021/acs.molpharmaceut.7b00069. Epub 2017 Jul 13.

Abstract

This study is focused on further understanding the characteristics of chitosan-N-acetylcysteine surface-modified nanostructured lipid carriers (CS-NAC-NLCs) in their interaction with ocular mucosa. Coumarin-6 (C6)-labeled NLCs, including uncoated NLCs, chitosan hydrochloride (CH)-, and CS-NAC-coated NLCs, were developed using a melt-emulsification technique and subsequently decorated with different types or portions of chitosan derivatives. Mucoadhesion was evaluated ex vivo using a flow-through process with fluorescence detection. The results demonstrated that the presence of CS-NAC on the C6-NLC surface provided the most obvious enhancement in adhesion due to the formation of both noncovalent (ionic) and covalent (disulfide bridges) interactions with mucus chains. Meanwhile, the concentration of CS-NAC in the formulation positively influenced the viscosity of the nanoparticles and hence prolonged their retention in the ocular tissue. Transcorneal penetration studies revealed that CS-NAC-NLC particles were able to penetrate through the entire corneal epithelium primarily via a transcellular route. The transport depth and velocity strongly relied on the modification material and the particle size. Ex vivo fluorescence imaging and in vivo ocular distribution investigations showed that C6 was broadly distributed in rabbit eye tissues and absorbed by aqueous humor after CS-NAC-NLC instillation. In relation to C6 eye drops, CS-NAC-NLCs achieved considerably higher C (4.01-fold), MRT (1.87-fold), and AUC (16.29-fold) in the aqueous humor. Moreover, the increase in drug absorption was greater in the cornea than in the conjunctiva. Thereby, it is possible to draw a conclusion that CS-NAC-NLCs presented great potential for drug application to the front portion of the eye.

摘要

本研究旨在进一步了解壳聚糖 - N - 乙酰半胱氨酸表面修饰的纳米结构脂质载体(CS - NAC - NLCs)与眼黏膜相互作用的特性。采用熔融乳化技术制备了香豆素 - 6(C6)标记的NLCs,包括未包衣的NLCs、壳聚糖盐酸盐(CH)包衣和CS - NAC包衣的NLCs,随后用不同类型或比例的壳聚糖衍生物进行修饰。采用荧光检测的流通法在体外评估黏膜黏附性。结果表明,C6 - NLC表面存在CS - NAC时,由于与黏液链形成非共价(离子)和共价(二硫键)相互作用,黏附性增强最为明显。同时,制剂中CS - NAC的浓度对纳米颗粒的黏度有积极影响,从而延长了它们在眼组织中的滞留时间。角膜透过性研究表明,CS - NAC - NLC颗粒主要通过跨细胞途径穿透整个角膜上皮。转运深度和速度强烈依赖于修饰材料和粒径。体外荧光成像和体内眼部分布研究表明,CS - NAC - NLC滴注后,C6广泛分布于兔眼组织并被房水吸收。与C6眼药水相比,CS - NAC - NLCs在房水中的C(4.01倍)、MRT(1.87倍)和AUC(16.29倍)显著更高。此外,角膜中的药物吸收增加比结膜中的更大。因此,可以得出结论,CS - NAC - NLCs在眼前部药物应用方面具有巨大潜力。

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