Preclinical Department, Faculty of Medicine, "Lucian Blaga" University of Sibiu, 550169 Sibiu, Romania.
Molecules. 2021 Oct 1;26(19):5976. doi: 10.3390/molecules26195976.
Gene-directed enzyme prodrug therapy (GDEPT) has been intensively studied as a promising new strategy of prodrug delivery, with its main advantages being represented by an enhanced efficacy and a reduced off-target toxicity of the active drug. In recent years, numerous therapeutic systems based on GDEPT strategy have entered clinical trials. In order to deliver the desired gene at a specific site of action, this therapeutic approach uses vectors divided in two major categories, viral vectors and non-viral vectors, with the latter being represented by chemical delivery agents. There is considerable interest in the development of non-viral vectors due to their decreased immunogenicity, higher specificity, ease of synthesis and greater flexibility for subsequent modulations. Dendrimers used as delivery vehicles offer many advantages, such as: nanoscale size, precise molecular weight, increased solubility, high load capacity, high bioavailability and low immunogenicity. The aim of the present work was to provide a comprehensive overview of the recent advances regarding the use of dendrimers as non-viral carriers in the GDEPT therapy.
基因导向酶前药疗法 (GDEPT) 已被深入研究,作为一种有前途的新前药递送策略,其主要优势在于增强了活性药物的疗效和降低了脱靶毒性。近年来,许多基于 GDEPT 策略的治疗系统已进入临床试验。为了在特定作用部位递送所需的基因,这种治疗方法使用分为两大类的载体,即病毒载体和非病毒载体,后者由化学递送剂代表。由于非病毒载体的免疫原性降低、特异性更高、易于合成以及对后续调节具有更大的灵活性,因此对其开发具有很大的兴趣。用作递送载体的树枝状聚合物具有许多优点,例如:纳米级尺寸、精确的分子量、增加的溶解度、高载药量、高生物利用度和低免疫原性。本工作的目的是全面概述树枝状聚合物作为非病毒载体在 GDEPT 治疗中的最新进展。
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