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壳聚糖水凝胶用于局部基因沉默。

Chitosan hydrogel for localized gene silencing.

机构信息

Department of Gynecologic Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.

出版信息

Cancer Biol Ther. 2011 May 1;11(9):839-45. doi: 10.4161/cbt.11.9.15185.

DOI:10.4161/cbt.11.9.15185
PMID:21358280
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3100632/
Abstract

OBJECTIVE

To achieve effective delivery of siRNA into target cells in vivo, we have developed a novel approach of siRNA delivery by using local drug delivery systems.

RESULTS

The chitosan hydrogel (CH-HG) displayed a liquid-solid phase transition in a temperature-dependent manner and formed an endothermic hydrogel in tumor tissue after intra-tumoral injection. Additionally, we tested the extent of in vivo delivery following a single intra-tumoral injection of Alexa555 siRNA/CH-HG into A375SM-bearing mice. The Alexa555 siRNA demonstrated higher localization into tumor cells compared to control. The Alexa555 siRNA delivery extends to tumor cells outside of CH-HG and some tumor cells also infiltrated into CH-HG. For therapeutic proof-of-concept studies, CH-HG including TG2-targeted siRNA significantly inhibited tumor growth in melanoma (A375SM) and breast (MDA-MB231) tumor models compared to control (A375SM: 72% reduction and MDA-MB231: 92% reduction, p < 0.001).

EXPERIMENTAL DESIGN

we prepared a CH-HG system loaded with siRNA to enhance localized therapeutic efficacy without risk for systemic side effects. Delivery of siRNA into CH-HG was confirmed by fluorescence microscopy. Antitumor efficacy was examined in mouse models of melanoma (A375SM) and breast (MDA-MD231) cancer.

CONCLUSIONS

This study developed a novel local delivery method for siRNA therapy using the CH-HG system. This approach could have broad applications for multiple localized diseases.

摘要

目的

为了实现 siRNA 在体内靶向细胞的有效传递,我们开发了一种利用局部药物递送系统递送 siRNA 的新方法。

结果

壳聚糖水凝胶(CH-HG)表现出温度依赖性的液-固相变,并在肿瘤内注射后在肿瘤组织中形成吸热水凝胶。此外,我们测试了单次肿瘤内注射 Alexa555siRNA/CH-HG 后体内递送的程度。与对照相比,Alexa555siRNA 显示出更高的肿瘤细胞定位。Alexa555siRNA 的递送范围扩展到 CH-HG 之外的肿瘤细胞,一些肿瘤细胞也渗透到 CH-HG 中。为了进行治疗概念验证研究,与对照相比,包含 TG2 靶向 siRNA 的 CH-HG 显著抑制了黑色素瘤(A375SM)和乳腺癌(MDA-MB231)肿瘤模型中的肿瘤生长(A375SM:减少 72%,MDA-MB231:减少 92%,p<0.001)。

实验设计

我们制备了负载 siRNA 的 CH-HG 系统,以增强局部治疗效果,同时避免全身副作用的风险。通过荧光显微镜证实了 siRNA 递送到 CH-HG 中。在黑色素瘤(A375SM)和乳腺癌(MDA-MD231)模型的小鼠中检查了抗肿瘤功效。

结论

本研究开发了一种使用 CH-HG 系统的新型局部 siRNA 治疗递送方法。这种方法可能有广泛的应用于多种局部疾病。

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