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局部递送 siRNA 采用可生物降解聚合物应用来增强 BMP 诱导的骨形成。

Local delivery of siRNA using a biodegradable polymer application to enhance BMP-induced bone formation.

机构信息

Department of Orthopaedic Surgery, Osaka City University Graduate School of Medicine, 1-4-3 Abenoku Asahimachi, Osaka 545-8585, Japan.

出版信息

Biomaterials. 2011 Dec;32(36):9642-8. doi: 10.1016/j.biomaterials.2011.08.026. Epub 2011 Oct 1.

DOI:10.1016/j.biomaterials.2011.08.026
PMID:21963281
Abstract

Small interfering RNA (siRNA) is useful tool for specific and efficient knockdown of disease-related genes. However, in vivo applications of siRNA are limited due to difficulty in its efficient delivery to target cells. In this study, we investigated the efficacy of a biodegradable hydrogel, poly-d,l-lactic acid-p-dioxanone-polyethylene glycol block co-polymer (PLA-DX-PEG), as a siRNA carrier. PLA-DX-PEG pellets with or without fluorescein-labeled dsRNA were implanted into mouse dosal muscle pouches. The cellular uptake of dsRNA surround the polymer was confirmed by fluorescent microscopy. The fluorescence intensity was dose-dependent of the dsRNA, and exhibited a time-dependent decrease. To investigate its biological efficiency, noggin (antagonoist to BMPs) gene-silencing with siRNA (siRNA/Noggin) was examined by the amount of suppression of BMP-2-induced noggin expression and the level of performance of BMP, indicated by ectopic bone formation. Noggin gene expression induced by BMP-2 was suppressed by addition of siRNA/Noggin to the implant, and the ectopic bone formation induced by implants with both BMP-2 and siRNA/Noggin was significantly greater than those induced by implants with BMP-2 alone. These results indicate the efficacy of local delivery of siRNAs by PLA-DX-PEG polymer, which intensified bone-inducing effects of BMP and promoted new bone formation by suppressing gene expression of Noggin.

摘要

小干扰 RNA(siRNA)是一种用于特异性和高效敲低疾病相关基因的有用工具。然而,由于其向靶细胞有效递送的困难,siRNA 的体内应用受到限制。在这项研究中,我们研究了可生物降解水凝胶聚-d,l-乳酸-p-二氧环己酮-聚乙二醇嵌段共聚物(PLA-DX-PEG)作为 siRNA 载体的功效。将带有或不带有荧光标记双链 RNA(dsRNA)的 PLA-DX-PEG 微球植入小鼠背部肌肉囊中。通过荧光显微镜证实了聚合物周围 dsRNA 的细胞摄取。荧光强度与 dsRNA 的剂量呈依赖性,并且表现出时间依赖性降低。为了研究其生物学效率,通过抑制 BMP-2 诱导的 noggin 表达量和 BMP 性能(由异位骨形成指示)来检查 noggin(BMPs 的拮抗剂)基因沉默与 siRNA(siRNA/Noggin)的关系。加入 siRNA/Noggin 可抑制 BMP-2 诱导的 noggin 基因表达,并且 BMP-2 和 siRNA/Noggin 共同植入物诱导的异位骨形成明显大于仅 BMP-2 诱导的植入物。这些结果表明 PLA-DX-PEG 聚合物局部递送 siRNA 的功效,其增强了 BMP 的诱导骨形成作用,并通过抑制 Noggin 的基因表达促进了新骨形成。

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