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首页> 外文期刊>Methods and findings in experimental and clinical pharmacology >Suppression of heart NF-kappaB p65 expression by jugular vein injection of RNAi in mice.
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Suppression of heart NF-kappaB p65 expression by jugular vein injection of RNAi in mice.

机译:颈静脉注射RNAi对小鼠心脏NF-κBp65表达的抑制作用。

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摘要

The nuclear factor-kappaB (NF-kappaB) in cardiac vascular endothelial cells (type II VEC) is a key factor that activates delayed xenograft rejection (DXR), and therefore inhibition of NF-kappaB gene expression may alleviate post-transplant rejection. siRNA technology was used to inhibit NF-kappaB p65 gene expression in ICR mice. After jugular vein injection of siRNA/in vivo-jetPEI complex, fluorescence levels of FAM-labeled siRNA in hearts and lungs were much higher after jugular vein injection than tail vein injection, suggesting more efficient siRNA delivery to the heart through the jugular vein. The amount of FAM fluorescence of hearts increased to the highest level between 48 and 72 hours after injection, and decreased gradually 1 week after injection. A minimum dose of 6 nmol NF-kappaB p65 siRNA and a siRNA/in vivo-jetPEI ratio of 6 (N/P = 6) were required for in vivo siRNA-mediated gene silencing in the heart. Under these conditions, application of siRNA/in vivo-jetPEI complexes from the jugular vein successfully suppressed NF-kappaB p65 expression in the heart. The same strategy can be applied to heart transplant animal models to protect against NF-kappaB gene-related type II VEC activation and xenograft rejection.
机译:心脏血管内皮细胞(II型VEC)中的核因子-kappaB(NF-kappaB)是激活延迟异种移植排斥(DXR)的关键因素,因此抑制NF-kappaB基因表达可以减轻移植后排斥反应。 siRNA技术用于抑制ICR小鼠中NF-κBp65基因的表达。颈静脉注射siRNA /体内-jetPEI复合物后,颈静脉注射后FAM标记的心和肺中siRNA的荧光水平比尾静脉注射高得多,这表明siRNA通过颈静脉向心脏的递送效率更高。注射后48至72小时之间,心脏的FAM荧光量增加至最高水平,注射后1周逐渐减少。心脏中的体内siRNA介导的基因沉默需要最低剂量的6 nmol NF-kappaB p65 siRNA和siRNA /体内-jetPEI比为6(N / P = 6)。在这些条件下,从颈静脉应用siRNA /体内-jetPEI复合物可成功抑制心脏中NF-κBp65的表达。可以将相同的策略应用于心脏移植动物模型,以防止NF-κB基因相关的II型VEC激活和异种移植排斥。

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