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Aerosol Delivery of siRNA to the Lungs. Part 1: Rationale for Gene Delivery Systems

机译:siRNA气雾剂递送至肺。第1部分:基因传递系统的原理

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摘要

This article reviews the pulmonary route of administration, aerosol delivery devices, characterization of pulmonary drug delivery systems, and discusses the rationale for inhaled delivery of siRNA. Diseases with known protein malfunctions may be mitigated through the use of siRNA therapeutics. The inhalation route of administration provides local delivery of siRNA therapeutics for the treatment of various pulmonary diseases, however barriers to pulmonary delivery and intracellular delivery of siRNA exists. siRNA loaded nanocarriers can be used to overcome the barriers associated with the pulmonary route, such as anatomical barriers, mucociliary clearance, and alveolar macrophage clearance. Apart from naked siRNA aerosol delivery, previously studied siRNA carrier systems comprise of lipidic, polymeric, peptide, or inorganic origin. Such siRNA delivery systems formulated as aerosols can be successfully delivered via an inhaler or nebulizer to the pulmonary region. Preclinical animal investigations of inhaled siRNA therapeutics rely on intratracheal and intranasal siRNA and siRNA nanocarrier delivery. Aerosolized siRNA delivery systems may be characterized using in vitro techniques, such as dissolution test, inertial cascade impaction, delivered dose uniformity assay, laser diffraction, and laser Doppler velocimetry. The ex vivo techniques used to characterize pulmonary administered formulations include the isolated perfused lung model. In vivo techniques like gamma scintigraphy, 3D SPECT, PET, MRI, fluorescence imaging and pharmacokinetic/pharmacodynamics analysis may be used for evaluation of aerosolized siRNA delivery systems. The use of inhalable siRNA delivery systems encounters barriers to their delivery, however overcoming the barriers while formulating a safe and effective delivery system will offer unique advances to the field of inhaled medicine.
机译:本文回顾了肺部给药途径,气雾剂输送装置,肺部药物输送系统的特性,并讨论了siRNA吸入输送的原理。具有已知蛋白质功能异常的疾病可以通过使用siRNA治疗剂来缓解。吸入给药途径提供了用于治疗各种肺部疾病的siRNA治疗剂的局部递送,但是存在肺递送和siRNA的细胞内递送的障碍。载有siRNA的纳米载体可用于克服与肺部途径相关的障碍,例如解剖学障碍,粘膜纤毛清除和肺泡巨噬细胞清除。除了裸露的siRNA气溶胶递送外,先前研究的siRNA载体系统还包含脂质,聚合物,肽或无机来源。配制为气雾剂的此类siRNA递送系统可通过吸入器或雾化器成功递送至肺区域。吸入siRNA治疗剂的临床前动物研究依赖于气管内和鼻内siRNA以及siRNA纳米载体的递送。可以使用体外技术来表征气雾化的siRNA递送系统,例如溶出度测试,惯性级联碰撞,递送剂量均匀性测定,激光衍射和激光多普勒测速仪。用于表征肺部给药制剂的离体技术包括分离的灌注肺模型。诸如伽马闪烁显像,3D SPECT,PET,MRI,荧光成像和药代动力学/药效学分析等体内技术可用于评估雾化的siRNA递送系统。吸入式siRNA传递系统的使用遇到了传递障碍,但是在制定安全有效的传递系统时克服这些障碍将为吸入药物领域带来独特的进步。

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