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具有可调表面性质的纳米载体,以打通系统药物和基因递送中的瓶颈。

Nanocarriers with tunable surface properties to unblock bottlenecks in systemic drug and gene delivery.

机构信息

Department of Pharmacy, School of Pharmaceutical Sciences, Sun Yat-sen University, University Town, Guangzhou 510006, PR China.

Department of Pharmacy, School of Pharmaceutical Sciences, Sun Yat-sen University, University Town, Guangzhou 510006, PR China.

出版信息

J Control Release. 2015 Sep 28;214:121-33. doi: 10.1016/j.jconrel.2015.07.014. Epub 2015 Jul 21.

Abstract

Nanocarrier-mediated drug and gene delivery systems hold great promise for providing more refined delivery (especially in cancer treatments) to maximize therapeutic efficacy while minimizing unfavorable side effects. Despite their promise, the highly effective transport of therapeutics in vivo remains a challenge. Over the last 20years, there has been a large amount of research directed toward the development of a multitude of nanocarriers for drug and gene delivery, but only a very small part has progressed into clinical trials. This suggests that the properties of current nanocarriers are not yet ideal for effective drug and gene delivery in vivo. Nanocarrier-mediated drug and gene delivery is a multi-step process, and inefficient delivery at any stage would ultimately result in an unsuccessful delivery. Unfortunately, existing nanocarriers with fixed surface properties, such as a PEGylated, cationized and bioconjugated surface, are not versatile enough to overcome the extracellular and intracellular barriers which require different surface properties. Consequently, their delivery efficacy is not optimal, leading to doubts and debates on the value of nanocarrier-based product development. To resolve the "fixed surface dilemma", the switchable surfaces of nanocarriers, which can surmount both extracellular and intracellular barriers, open up the possibility of highly efficient delivery in vivo. Here, we review and highlight the recent developments in the design of nanocarrier delivery systems with tunable surface properties in response to microenvironment triggers. Strategies including zwitterionic nanocarriers, polymer brushes, layer-by-layer nanocarriers and cleavable conjugated nanocarriers are presented. These representative examples and their respective outcomes elaborate the benefits and efficiencies of these nanocarriers at the individual stages of drug and gene delivery.

摘要

纳米载体介导的药物和基因传递系统在提供更精细的传递(特别是在癌症治疗中)方面具有很大的潜力,可以最大限度地提高治疗效果,同时最大限度地减少不利的副作用。尽管它们有很大的前景,但在体内实现治疗药物的高效输送仍然是一个挑战。在过去的 20 年中,已经有大量的研究致力于开发多种用于药物和基因传递的纳米载体,但只有一小部分进展到临床试验阶段。这表明,目前纳米载体的特性对于体内有效的药物和基因传递还不是理想的。纳米载体介导的药物和基因传递是一个多步骤的过程,任何阶段的低效传递最终都会导致传递失败。不幸的是,具有固定表面特性的现有纳米载体,如 PEG 化、阳离子化和生物共轭表面,不够通用,无法克服需要不同表面特性的细胞外和细胞内障碍。因此,它们的传递效果不是最佳的,导致对基于纳米载体的产品开发的价值产生怀疑和争议。为了解决“固定表面困境”,纳米载体的可切换表面可以克服细胞外和细胞内的障碍,为体内高效传递开辟了可能性。在这里,我们综述并强调了最近在设计具有响应微环境触发的可调表面特性的纳米载体传递系统方面的进展。提出了包括两性离子纳米载体、聚合物刷、层层纳米载体和可裂解共轭纳米载体的策略。这些代表性的例子及其各自的结果详细阐述了这些纳米载体在药物和基因传递各个阶段的优势和效率。

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