A Direct In Vivo RNAi Screen Identifies MKK4 as a Key Regulator of Liver Regeneration

The liver harbors a distinct capacity for endogenous regeneration; however, liver regeneration is often impaired in disease and therefore insufficient to compensate for the loss of hepatocytes and organ function. Here we describe a functional genetic approach for the identification of gene targets t...

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Published inCell Vol. 153; no. 2; pp. 389 - 401
Main Authors Wuestefeld, Torsten, Pesic, Marina, Rudalska, Ramona, Dauch, Daniel, Longerich, Thomas, Kang, Tae-Won, Yevsa, Tetyana, Heinzmann, Florian, Hoenicke, Lisa, Hohmeyer, Anja, Potapova, Anna, Rittelmeier, Ina, Jarek, Michael, Geffers, Robert, Scharfe, Maren, Klawonn, Frank, Schirmacher, Peter, Malek, Nisar P., Ott, Michael, Nordheim, Alfred, Vogel, Arndt, Manns, Michael P., Zender, Lars
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 11.04.2013
Subjects
animal models
Animals
Cell Cycle
Cell Differentiation
DNA Transposable Elements
Fibrosis
Gene Knockdown Techniques
genes
hepatocytes
Hepatocytes - cytology
Hepatocytes - physiology
Hydrolases - genetics
Hydrolases - metabolism
liver
Liver - cytology
Liver - injuries
Liver - pathology
Liver - physiology
liver failure
liver regeneration
MAP Kinase Kinase 4 - antagonists & inhibitors
MAP Kinase Kinase 4 - genetics
MAP Kinase Kinase 4 - metabolism
Mice
RNA
RNA Interference
RNA, Small Interfering - metabolism
transcription factors
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Summary:The liver harbors a distinct capacity for endogenous regeneration; however, liver regeneration is often impaired in disease and therefore insufficient to compensate for the loss of hepatocytes and organ function. Here we describe a functional genetic approach for the identification of gene targets that can be exploited to increase the regenerative capacity of hepatocytes. Pools of small hairpin RNAs (shRNAs) were directly and stably delivered into mouse livers to screen for genes modulating liver regeneration. Our studies identify the dual-specific kinase MKK4 as a master regulator of liver regeneration. MKK4 silencing robustly increased the regenerative capacity of hepatocytes in mouse models of liver regeneration and acute and chronic liver failure. Mechanistically, induction of MKK7 and a JNK1-dependent activation of the AP1 transcription factor ATF2 and the Ets factor ELK1 are crucial for increased regeneration of hepatocytes with MKK4 silencing. [Display omitted] ► Direct in vivo RNAi screening for modulators of liver regeneration is feasible ► Identification of MKK4 as a master regulator of liver regeneration ► MKK4 is a potential therapeutic target in acute and chronic liver disease ► ATF2 and ELK1 are essential downstream factors in MKK4-silenced hepatocytes An in vivo functional genetic screen identifies MKK4 as a master regulator of liver regeneration in models of acute and chronic liver disease.
Bibliography:http://dx.doi.org/10.1016/j.cell.2013.03.026
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ISSN:0092-8674
1097-4172
DOI:10.1016/j.cell.2013.03.026