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疏水修饰的小干扰RNA在原代神经元和小鼠大脑中沉默亨廷顿蛋白mRNA

Hydrophobically Modified siRNAs Silence Huntingtin mRNA in Primary Neurons and Mouse Brain.

作者信息

Alterman Julia F, Hall Lauren M, Coles Andrew H, Hassler Matthew R, Didiot Marie-Cecile, Chase Kathryn, Abraham Jasmin, Sottosanti Emily, Johnson Emily, Sapp Ellen, Osborn Maire F, Difiglia Marian, Aronin Neil, Khvorova Anastasia

机构信息

RNA Therapeutics Institute, University of Massachusetts Medical School, Worcester, Massachusetts, USA.

Department of Molecular Medicine, University of Massachusetts Medical School, Worcester, Massachusetts, USA.

出版信息

Mol Ther Nucleic Acids. 2015 Dec 1;4(12):e266. doi: 10.1038/mtna.2015.38.

Abstract

Applications of RNA interference for neuroscience research have been limited by a lack of simple and efficient methods to deliver oligonucleotides to primary neurons in culture and to the brain. Here, we show that primary neurons rapidly internalize hydrophobically modified siRNAs (hsiRNAs) added directly to the culture medium without lipid formulation. We identify functional hsiRNAs targeting the mRNA of huntingtin, the mutation of which is responsible for Huntington's disease, and show that direct uptake in neurons induces potent and specific silencing in vitro. Moreover, a single injection of unformulated hsiRNA into mouse brain silences Htt mRNA with minimal neuronal toxicity. Thus, hsiRNAs embody a class of therapeutic oligonucleotides that enable simple and straightforward functional studies of genes involved in neuronal biology and neurodegenerative disorders in a native biological context.

摘要

RNA干扰在神经科学研究中的应用一直受到限制,因为缺乏简单有效的方法将寡核苷酸递送至培养的原代神经元以及大脑中。在此,我们表明原代神经元能够快速内化直接添加到培养基中而无需脂质制剂的疏水修饰小干扰RNA(hsiRNA)。我们鉴定出靶向亨廷顿蛋白mRNA的功能性hsiRNA,其突变会导致亨廷顿舞蹈症,并且表明在神经元中直接摄取可在体外诱导有效且特异性的沉默。此外,向小鼠脑内单次注射未配制的hsiRNA可使Htt mRNA沉默,同时神经元毒性最小。因此,hsiRNA体现了一类治疗性寡核苷酸,能够在天然生物学环境中对参与神经元生物学和神经退行性疾病的基因进行简单直接的功能研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3140/5014532/19f4d0cd976e/mtna201538f1.jpg

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