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    RNAi-nanoparticulate manipulation of gene expression as a new functional genomics tool in the liver

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    Authors
    Yin, Hao
    Bogorad, Roman L.
    Barnes, Carmen
    Walsh, Stephen
    Zhuang, Iris
    Nonaka, Hidenori
    Ruda, Vera
    Kuchimanchi, Satya
    Nechev, Lubomir
    Akinc, Akin
    Xue, Wen
    Zerial, Marino
    Langer, Robert
    Anderson, Daniel G.
    Koteliansky, Victor
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    UMass Chan Affiliations
    Program in Molecular Medicine
    RNA Therapeutics Institute
    Document Type
    Journal Article
    Publication Date
    2016-04-01
    Keywords
    Biochemistry, Biophysics, and Structural Biology
    Cell and Developmental Biology
    Genetics and Genomics
    Hepatology
    Therapeutics
    
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    Link to Full Text
    https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5381270/
    Abstract
    BACKGROUND and AIMS: The Hippo pathway controls organ size through a negative regulation of the transcription co-activator Yap1. The overexpression of hyperactive mutant Yap1 or deletion of key components in the Hippo pathway leads to increased organ size in different species. Analysis of interactions of this pathway with other cellular signals corroborating organ size control is limited in part due to the difficulties associated with development of rodent models. METHODS: Here, we develop a new model of reversible induction of the liver size in mice using siRNA-nanoparticles targeting two kinases of the Hippo pathway, namely, mammalian Ste20 family kinases 1 and 2 (Mst1 and Mst2), and an upstream regulator, neurofibromatosis type II (Nf2). RESULTS: The triple siRNAs nanoparticle-induced hepatomegaly in mice phenocopies one observed with Mst1(-/-)Mst2(-/-) liver-specific depletion, as shown by extensive proliferation of hepatocytes and activation of Yap1. The simultaneous co-treatment with a fourth siRNA nanoparticle against Yap1 fully blocked the liver growth. Hippo pathway-induced liver enlargement is associated with p53 activation, evidenced by its accumulation in the nuclei and upregulation of its target genes. Moreover, injections of the triple siRNAs nanoparticle in p53(LSL/LSL) mice shows that livers lacking p53 expression grow faster and exceed the size of livers in p53 wild-type animals, indicating a role of p53 in controlling Yap1-induced liver growth. CONCLUSION: Our data show that siRNA-nanoparticulate manipulation of gene expression can provide the reversible control of organ size in adult animals, which presents a new avenue for the investigation of complex regulatory networks in liver.
    Source

    J Hepatol. 2016 Apr;64(4):899-907. doi: 10.1016/j.jhep.2015.11.028. Epub 2015 Nov 30. Link to article on publisher's site

    DOI
    10.1016/j.jhep.2015.11.028
    Permanent Link to this Item
    http://hdl.handle.net/20.500.14038/48806
    PubMed ID
    26658687
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    Link to Article in PubMed

    ae974a485f413a2113503eed53cd6c53
    10.1016/j.jhep.2015.11.028
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