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Microneedle-based drug delivery systems: Microfabrication, drug delivery, and safety.

机译:基于微针的药物输送系统:微细加工,药物输送和安全性。

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摘要

Many promising therapeutic agents are limited by their inability to reach the systemic circulation, due to the excellent barrier properties of biological membranes, such as the stratum corneum (SC) of the skin or the sclera/cornea of the eye and others. The outermost layer of the skin, the SC, is the principal barrier to topically-applied medications. The intact SC thus provides the main barrier to exogenous substances, including drugs. Only drugs with very specific physicochemical properties (molecular weight < 500 Da, adequate lipophilicity, and low melting point) can be successfully administered transdermally. Transdermal delivery of hydrophilic drugs and macromolecular agents of interest, including peptides, DNA, and small interfering RNA is problematic. Therefore, facilitation of drug penetration through the SC may involve by-pass or reversible disruption of SC molecular architecture. Microneedles (MNs), when used to puncture skin, will by-pass the SC and create transient aqueous transport pathways of micron dimensions and enhance the transdermal permeability. These micropores are orders of magnitude larger than molecular dimensions, and, therefore, should readily permit the transport of hydrophilic macromolecules. Various strategies have been employed by many research groups and pharmaceutical companies worldwide, for the fabrication of MNs. This review details various types of MNs, fabrication methods and, importantly, investigations of clinical safety of MN.
机译:由于生物膜例如皮肤的角质层(SC)或眼睛的巩膜/角膜等的生物膜的优异屏障性能,许多有前途的治疗剂由于无法达到体循环而受到限制。皮肤的最外层,即SC,是局部应用药物的主要障碍。完整的SC因此为包括药物在内的外源物质提供了主要屏障。只有具有非常特殊的理化特性(分子量<500 Da,足够的亲脂性和低熔点)的药物才能成功地经皮给药。亲水性药物和感兴趣的大分子药物(包括肽,DNA和小的干扰RNA)的透皮递送是有问题的。因此,促进药物通过SC的渗透可能涉及SC分子结构的旁路或可逆破坏。当用于穿刺皮肤时,微针(MNs)将绕过SC,并形成微米级的瞬时水传输路径,并增强透皮渗透性。这些微孔比分子尺寸大几个数量级,因此,应易于允许亲水性大分子的运输。全球许多研究小组和制药公司已采用各种策略来制造MN。这篇综述详细介绍了各种类型的MN,制造方法以及重要的是MN临床安全性的研究。

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