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用于眼部给药的储库植入物中RNA纳米颗粒的持续释放。

Sustained release of RNA nanoparticles from reservoir implant for ocular delivery.

作者信息

Shi Zhanquan, Zhong Cheng, Binzel Daniel W, Jin Kai, Guo Peixuan, Li S Kevin

机构信息

Division of Pharmaceutical Sciences, College of Pharmacy, University of Cincinnati, Cincinnati, OH 45267, United States.

Center for RNA Nanobiotechnology and Nanomedicine, College of Pharmacy, James Comprehensive Cancer Center, The Ohio State University, Columbus, OH 43210, United States.

出版信息

J Pharm Sci. 2025 Feb;114(2):1423-1433. doi: 10.1016/j.xphs.2024.12.019. Epub 2024 Dec 24.

Abstract

Previous studies of RNA nanoparticles have demonstrated the potential of these nanoparticles in ocular delivery via the subconjunctival route. Sustained ocular delivery is beneficial for chronic eye disease treatment, and utilizing a reservoir implant in the periocular space (e.g., episcleral implant) can prolong ocular delivery of these nanoparticles. The objectives of the present study were to (a) demonstrate the fabrication of the reservoir implants, (b) evaluate the performance of the implants with model permeants and RNA nanoparticles in vitro, and (c) investigate the applicability of hindered transport theory for the release kinetics from the implants. In vitro release testing was performed with the implants to determine the release kinetics and implant membrane permeability. In addition to RNA nanoparticles, model permeants fluorescein-isothiocyanate (FITC) labeled dextrans (10, 40, and 150 kDa) were examined. The results indicated that the rates of permeant release from the implants were a function of the (a) size and structure of the permeant/nanoparticle and (b) type and pore size of the implant membrane. The model analyses provided insights into implant membrane transport and ocular pharmacokinetics of the nanoparticles for transscleral delivery. The results suggested the potential of prolonged delivery of the RNA nanoparticles with the episcleral implant approach.

摘要

先前对RNA纳米颗粒的研究已经证明了这些纳米颗粒通过结膜下途径进行眼部给药的潜力。持续的眼部给药有利于慢性眼病的治疗,在眼周空间使用储库植入物(例如巩膜上植入物)可以延长这些纳米颗粒的眼部给药时间。本研究的目的是:(a)展示储库植入物的制造过程;(b)在体外评估植入物与模型渗透剂和RNA纳米颗粒的性能;(c)研究阻碍传输理论对植入物释放动力学的适用性。对植入物进行体外释放测试,以确定释放动力学和植入物膜的通透性。除了RNA纳米颗粒外,还检测了模型渗透剂异硫氰酸荧光素(FITC)标记的葡聚糖(10、40和150 kDa)。结果表明,植入物中渗透剂的释放速率取决于:(a)渗透剂/纳米颗粒的大小和结构;(b)植入物膜的类型和孔径。模型分析为纳米颗粒经巩膜给药的植入物膜转运和眼部药代动力学提供了见解。结果表明,巩膜上植入物方法具有延长RNA纳米颗粒给药时间的潜力。

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