Literature DB >> 20697157

Argonaute proteins are key determinants of RNAi efficacy, toxicity, and persistence in the adult mouse liver.

Dirk Grimm1, Lora Wang, Joyce S Lee, Nina Schürmann, Shuo Gu, Kathleen Börner, Theresa A Storm, Mark A Kay.   

Abstract

shRNA overexpression from viral gene therapy vectors can trigger cytotoxicity leading to organ failure and lethality in mice and rats. This process likely involves saturation of endogenous cellular RNAi factors including exportin-5 (Xpo-5). Here, we have shown that Xpo-5 overexpression enhanced shRNA efficiency in the liver of adult mice but increased hepatotoxicity. We identified the 4 members of the human Argonaute (Ago) protein family as downstream factors involved in saturation of endogenous cellular RNAi, all of which were able to interact with shRNAs in cells and mice. In Ago/shRNA coexpression studies, Ago-2 (Slicer) was the primary rate-limiting determinant of both in vitro and in vivo RNAi efficacy, toxicity, and persistence. In adult mice, vector-based Ago-2/Xpo-5 coexpression enhanced U6-driven shRNA silencing of exogenous and endogenous hepatic targets, reduced hepatotoxicity, and extended RNAi stability by more than 3 months. Use of weaker RNA polymerase III promoters to minimize shRNA expression likewise alleviated in vivo toxicity and permitted greater than 95% persistent knockdown of hepatitis B virus and other transgenes in mouse liver for more than 1 year. Our studies substantiate that abundant small RNAs can overload the endogenous RNAi pathway and reveal possible strategies for reducing hepatotoxicity of short- and long-term clinical gene silencing in humans.

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Year:  2010        PMID: 20697157      PMCID: PMC2929739          DOI: 10.1172/JCI43565

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  68 in total

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3.  Positional effects of short interfering RNAs targeting the human coagulation trigger Tissue Factor.

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4.  Increased maintenance and persistence of transgenes by excision of expression cassettes from plasmid sequences in vivo.

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5.  Evidence of RNAi in humans from systemically administered siRNA via targeted nanoparticles.

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6.  Minimizing variables among hairpin-based RNAi vectors reveals the potency of shRNAs.

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7.  Low-level shRNA cytotoxicity can contribute to MYC-induced hepatocellular carcinoma in adult mice.

Authors:  Shelly Beer; David I Bellovin; Joyce S Lee; Kimberly Komatsubara; Lora S Wang; Huishan Koh; Kathleen Börner; Theresa A Storm; Corrine R Davis; Mark A Kay; Dean W Felsher; Dirk Grimm
Journal:  Mol Ther       Date:  2009-10-20       Impact factor: 11.454

8.  Short-interfering-RNA-mediated gene silencing in mammalian cells requires Dicer and eIF2C translation initiation factors.

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Journal:  PLoS One       Date:  2008-03-05       Impact factor: 3.240

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  99 in total

1.  In vivo delivery of cytoplasmic RNA virus-derived miRNAs.

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Review 3.  Action and reaction: the biological response to siRNA and its delivery vehicles.

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Review 6.  RNA interference and cancer therapy.

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7.  Argonaute protein as a linker to command center of physiological processes.

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Review 8.  Lentiviral vector-mediated RNA silencing in the central nervous system.

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10.  Triple combination of siRNAs targeting TGFβ1, TGFβR2, and CTGF enhances reduction of collagen I and smooth muscle actin in corneal fibroblasts.

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