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低聚乳酸纳米颗粒增强组织靶向性:以贝达喹啉在结核性心包炎中向心脏组织的控释为例

Oligosaccharide Lactate Nanoparticles Enhance Tissue Targeting: A Case Study of the Controlled Delivery of Bedaquiline to Cardiac Tissue in TB Pericarditis.

作者信息

Ayodele Simisola, Kumar Pradeep, van Eyk Armorel, van der Bijl Pieter, Choonara Yahya E

机构信息

Wits Advanced Drug Delivery Platform Research Unit, Department of Pharmacy and Pharmacology, School of Therapeutic Sciences, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg 2193, South Africa.

Department of Pharmacy and Pharmacology, School of Therapeutic Sciences, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg 2193, South Africa.

出版信息

Molecules. 2025 Jul 3;30(13):2845. doi: 10.3390/molecules30132845.

Abstract

Bedaquiline is known to shorten the duration of therapy of tuberculosis but has limitations, e.g., poor solubility and adverse effects such as prolongation of the QT interval. In this study, bedaquiline was incorporated into an inherently targeted nanosystem for improved permeation of the drug, with ex vivo diffusion studies performed to investigate its penetration. The bedaquiline-loaded mannan-chitosan oligosaccharide lactate nanoparticles were prepared by a one-step ionic gelation probe sonication method. A PermeGear 7-in-line flow-through diffusion system was used for the ex vivo diffusion studies across porcine and human pericardia. Bedaquiline-loaded nanoparticles with a particle size and potential of 192.4 nm and 40.5 mV, respectively, were obtained. The drug-loaded mannan-chitosan nanoparticles had an encapsulation efficacy of 98.7% and drug loading of 0.6%. Diffusion data indicated a steady-state flux of 2.889 and 2.346 µg.cm.min for porcine and human pericardia, respectively. The apparent permeability coefficients were calculated to be 2.66 × 10 cm.min and 2.16 × 10 cm.min for porcine and human pericardia, respectively. The lag phases were 52.72 min and 0 min for porcine and human pericardia, respectively. The drug permeation indicated a consistent and linear diffusion pattern across both porcine and human pericardia, additionally approving the porcine pericardium as a great comparable tissue to human tissue for pericardial studies. This study is the first to demonstrate ex vivo diffusion of bedaquiline-loaded, macrophage-targeted chitosan-mannan nanoparticles across both human and porcine pericardia, representing a novel platform for disease-targeted, localized treatment of TB pericarditis.

摘要

已知贝达喹啉可缩短结核病的治疗疗程,但存在局限性,例如溶解度差以及会产生如QT间期延长等不良反应。在本研究中,将贝达喹啉载入一种具有内在靶向性的纳米系统以改善药物渗透,并进行了体外扩散研究以考察其渗透性。采用一步离子凝胶探针超声法制备了载贝达喹啉的甘露聚糖-壳寡糖乳酸盐纳米粒。使用PermeGear 7通道流通扩散系统进行跨猪心包和人心包的体外扩散研究。获得了粒径和电位分别为192.4 nm和40.5 mV的载贝达喹啉纳米粒。载药甘露聚糖-壳聚糖纳米粒的包封率为98.7%,载药量为0.6%。扩散数据表明,猪心包和人心包的稳态通量分别为2.889和2.346 μg·cm·min。计算得到猪心包和人心包的表观渗透系数分别为2.66×10 cm·min和2.16×10 cm·min。猪心包和人心包的滞后时间分别为52.72 min和零分钟。药物渗透表明在猪心包和人心包上均呈现一致且线性的扩散模式,此外还证实了猪心包是用于心包研究的与人组织极具可比性的组织。本研究首次证明了载贝达喹啉、巨噬细胞靶向的壳聚糖-甘露聚糖纳米粒在人和猪心包上的体外扩散,代表了一种用于结核病心包炎疾病靶向局部治疗的新型平台。

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