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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Dexamethasone-loaded peptide micelles for delivery of the heme oxygenase-1 gene to ischemic brain
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Dexamethasone-loaded peptide micelles for delivery of the heme oxygenase-1 gene to ischemic brain

机译:负载地塞米松的肽微团可将血红素加氧酶-1基因传递至缺血性脑

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摘要

The R3V6 peptides, which are composed of a 3-arginine block and a 6-valine block, formed self-assembled micelles in aqueous solution. Dye quenching assays showed that a hydrophobic fluorescent dye, 5-dodecanoylaminofluorescein (DAF), interacted with and was loaded into the hydrophobic core of the micelles. In this study, dexamethasone-loaded R3V6 peptide micelles (R3V6-Dexa) were evaluated as a gene carrier. R3V6-Dexa had higher gene delivery efficiency in human embryonic kidney 293 cells compared to those of the R3V6 peptides and poly-l-lysine (PLL). Dexamethasone might stabilize the micelle structure of the R3V6 peptides by forming strong hydrophobic cores and enhanced the transfection efficiency. Furthermore, R3V6-Dexa reduced the expression of an inflammatory cytokine, interleukin-6 (IL-6), more efficiently in lipopolysaccharide (LPS)-induced Raw264.7 cells than did dexamethasone, suggesting that R3V6-Dexa is also a useful carrier for dexamethasone delivery. A focal brain ischemia-reperfusion model was produced by middle cerebral artery occlusion (MCAO). A heme oxygenase-1 (HO-1) expression plasmid DNA, pSV-HO-1, was delivered into the brain using R3V6-Dexa as a carrier. The pSV-HO-1/R3V6-Dexa complex was injected into the brain 1 hr prior to MCAO. Twenty-four hours later, the HO-1 expression of the pSV-HO-1/R3V6-Dexa injection group was higher than those of the MCAO control, pβ-Luc/R3V6-Dexa, and pSV-HO-1/PEI25k injection groups. In addition, the infarct size was reduced due to the delivery of pSV-HO-1/R3V6-Dexa complex. Therefore, R3V6-Dexa may be a useful carrier for HO-1 gene delivery and stroke gene therapy.
机译:由3-精氨酸嵌段和6-缬氨酸嵌段组成的R3V6肽在水溶液中形成自组装胶束。染料淬灭试验表明,疏水荧光染料5-十二烷酰氨基荧光素(DAF)与微团的疏水核心相互作用并被加载到其中。在这项研究中,地塞米松负载的R3V6肽胶束(R3V6-Dexa)被评估为基因载体。与R3V6肽和聚-1-赖氨酸(PLL)相比,R3V6-Dexa在人胚胎肾293细胞中具有更高的基因传递效率。地塞米松可能通过形成强疏水核心并提高转染效率来稳定R3V6肽的胶束结构。此外,与地塞米松相比,R3V6-Dexa在脂多糖(LPS)诱导的Raw264.7细胞中更有效地降低了炎性细胞因子白细胞介素6(IL-6)的表达,这表明R3V6-Dexa也是一种有用的载体地塞米松递送。通过大脑中动脉闭塞(MCAO)产生局灶性脑缺血再灌注模型。使用R3V6-Dexa作为载体,将血红素加氧酶-1(HO-1)表达质粒DNA pSV-HO-1传递到大脑中。在MCAO之前1小时,将pSV-HO-1 / R3V6-Dexa复合物注入大脑。 24小时后,pSV-HO-1 / R3V6-Dexa注射组的HO-1表达高于MCAO对照,pβ-Luc/ R3V6-Dexa和pSV-HO-1 / PEI25k注射组的HO-1表达。组。另外,由于递送pSV-HO-1 / R3V6-Dexa复合物,梗塞面积减小。因此,R3V6-Dexa可能是HO-1基因传递和中风基因治疗的有用载体。

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