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Transvascular delivery of small interfering RNA to the central nervous system

机译:小干扰RNA的血管内输送至中枢神经系统

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A major impediment in the treatment of neurological diseases is the presence of the blood-brain barrier, which precludes the entry of therapeutic molecules from blood to brain. Here we show that a short peptide derived from rabies virus glycoprotein (RVG) enables the transvascular delivery of small interfering RNA (siRNA) to the brain. This 29-amino-acid peptide specifically binds to the acetylcholine receptor expressed by neuronal cells. To enable siRNA binding, a chimaeric peptide was synthesized by adding nonamer arginine residues at the carboxy terminus of RVG. This RVG-9R peptide was able to bind and transduce siRNA to neuronal cells in vitro, resulting in efficient gene silencing. After intravenous injection into mice, RVG-9R delivered siRNA to the neuronal cells, resulting in specific gene silencing within the brain. Furthermore, intravenous treatment with RVG-9R-bound antiviral siRNA afforded robust protection against fatal viral encephalitis in mice. Repeated administration of RVG-9R-bound siRNA did not induce inflammatory cytokines or anti-peptide antibodies. Thus, RVG-9R provides a safe and noninvasive approach for the delivery of siRNA and potentially other therapeutic molecules across the blood-brain barrier.
机译:治疗神经系统疾病的主要障碍是血脑屏障的存在,它阻止了治疗分子从血液进入大脑。在这里,我们显示了源自狂犬病病毒糖蛋白(RVG)的短肽能够将小干扰RNA(siRNA)跨血管输送到大脑。这种29个氨基酸的肽与神经元细胞表达的乙酰胆碱受体特异性结合。为了使siRNA结合,通过在RVG的羧基末端添加九聚精氨酸残基来合成嵌合肽。该RVG-9R肽能够在体外结合siRNA并将其转导至神经元细胞,从而实现有效的基因沉默。向小鼠静脉注射后,RVG-9R将siRNA传递至神经元细胞,导致大脑内特定基因沉默。此外,用RVG-9R结合的抗病毒siRNA进行静脉内治疗可对小鼠致命的病毒性脑炎提供强有力的保护。重复给予RVG-9R结合的siRNA不会诱导炎性细胞因子或抗肽抗体。因此,RVG-9R为跨血脑屏障递送siRNA和潜在的其他治疗分子提供了一种安全且无创的方法。

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