The transcription factor c‐Jun protects against sustained hepatic endoplasmic reticulum stress thereby promoting hepatocyte survival
Identifieur interne : 001329 ( Main/Exploration ); précédent : 001328; suivant : 001330The transcription factor c‐Jun protects against sustained hepatic endoplasmic reticulum stress thereby promoting hepatocyte survival
Auteurs : Matthias Fuest [Allemagne] ; Karolina Willim [Allemagne] ; Sabine Macnelly [Allemagne] ; Nicole Fellner [Autriche] ; Guenter P. Resch [Autriche] ; Hubert E. Blum [Allemagne] ; Peter Hasselblatt [Allemagne]Source :
- Hepatology [ 0270-9139 ] ; 2012-02.
English descriptors
- Teeft :
- Acute hepatitis, Apoptosis, Aspartate aminotransferase, Autophagosome numbers, Autophagy, Biol, Biol chem, Calcium homeostasis, Caspase cleavage, Cell biol, Cell damage, Cell death, Cell survival, Cellular redox state, Control mice, Cytoplasmic, Cytoplasmic vacuolization, Endoplasmic, Endoplasmic reticulum, Endoplasmic reticulum stress, Fuest, Functional impact, Genotype, Hepatic, Hepatic expression, Hepatic steatosis, Hepatocyte, Hepatocyte damage, Hepatocyte fate, Hepatocyte survival, Hepatocytes, Hepatology, Hepatoma cells, Human hepg2, Immunoblot, Immunoblot analysis, Important regulator, Important regulators, Important step, Inducible nitric oxide synthase, Insulin resistance, Intraperitoneal injection, Kinase, Kinase inhibitor, Knockout mice, Lactate dehydrogenase, Lc3b abcam, Liver diseases, Massive cytoplasmic vacuolization, Methods enzymol, More detail, Mrna expression, Ndings, Oxidative, Oxidative stress, Pancreatic beta cells, Parental cell line, Pathway, Phagophore expansion, Pharmacological inhibition, Phase contrast images, Phenotype, Plos biol, Primary mouse hepatocytes, Profound cytoplasmic vacuolization, Protein expression, Protein response, Protein synthesis, Regulator, Relative expression, Reticulum, Robust induction, Small inserts, Stress response, Stress responses, Stress results, Strong inducer, Subsequent cell death, Target gene, Timepoints, Transcription, Transcription factor, Transgenic mice, Transmission electron microscopy, University hospital freiburg, Untreated, Untreated control cells, Untreated control livers, Vacuolization.
Abstract
Endoplasmic reticulum (ER) stress due to accumulation of hepatoviral or misfolded proteins is increasingly recognized as an important step in the pathogenesis of inflammatory, toxic, and metabolic liver diseases. ER stress results in the activation of several intracellular signaling pathways including Jun N‐terminal kinase (JNK). The AP‐1 (activating protein 1) transcription factor c‐Jun is a prototypic JNK target and important regulator of hepatocyte survival, proliferation, and liver tumorigenesis. Because the functions of c‐Jun during the ER stress response are poorly understood, we addressed this issue in primary hepatocytes and livers of hepatocyte‐specific c‐Jun knockout mice. ER stress was induced pharmacologically in vitro and in vivo and resulted in a rapid and robust induction of c‐Jun protein expression. Interestingly, ER‐stressed hepatocytes lacking c‐Jun displayed massive cytoplasmic vacuolization due to ER distension. This phenotype correlated with exacerbated and sustained activation of canonical ER stress signaling pathways. Moreover, sustained ER stress in hepatocytes lacking c‐Jun resulted in increased cell damage and apoptosis. ER stress is also a strong inducer of macroautophagy, a cell‐protective mechanism of self‐degradation of cytoplasmic components and organelles. Interestingly, autophagosome numbers in response to ER stress were reduced in hepatocytes lacking c‐Jun. To further validate these findings, macroautophagy was inhibited chemically in ER‐stressed wildtype hepatocytes, which resulted in cytoplasmic vacuolization and increased cell damage closely resembling the phenotypes observed in c‐Jun‐deficient cells. Conclusion: Our findings indicate that c‐Jun protects hepatocytes against excessive activation of the ER stress response and subsequent cell death and provide evidence that c‐Jun functionally links ER stress responses and macroautophagy. (HEPATOLOGY 2012)
Url:
DOI: 10.1002/hep.24699
Affiliations:
- Allemagne, Autriche
- Bade-Wurtemberg, District de Fribourg-en-Brisgau, Vienne (Autriche)
- Fribourg-en-Brisgau, Vienne (Autriche)
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expression</term><term>Hepatic steatosis</term><term>Hepatocyte</term><term>Hepatocyte damage</term><term>Hepatocyte fate</term><term>Hepatocyte survival</term><term>Hepatocytes</term><term>Hepatology</term><term>Hepatoma cells</term><term>Human hepg2</term><term>Immunoblot</term><term>Immunoblot analysis</term><term>Important regulator</term><term>Important regulators</term><term>Important step</term><term>Inducible nitric oxide synthase</term><term>Insulin resistance</term><term>Intraperitoneal injection</term><term>Kinase</term><term>Kinase inhibitor</term><term>Knockout mice</term><term>Lactate dehydrogenase</term><term>Lc3b abcam</term><term>Liver diseases</term><term>Massive cytoplasmic vacuolization</term><term>Methods enzymol</term><term>More detail</term><term>Mrna expression</term><term>Ndings</term><term>Oxidative</term><term>Oxidative stress</term><term>Pancreatic beta cells</term><term>Parental cell line</term><term>Pathway</term><term>Phagophore 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type="abstract" xml:lang="en">Endoplasmic reticulum (ER) stress due to accumulation of hepatoviral or misfolded proteins is increasingly recognized as an important step in the pathogenesis of inflammatory, toxic, and metabolic liver diseases. ER stress results in the activation of several intracellular signaling pathways including Jun N‐terminal kinase (JNK). The AP‐1 (activating protein 1) transcription factor c‐Jun is a prototypic JNK target and important regulator of hepatocyte survival, proliferation, and liver tumorigenesis. Because the functions of c‐Jun during the ER stress response are poorly understood, we addressed this issue in primary hepatocytes and livers of hepatocyte‐specific c‐Jun knockout mice. ER stress was induced pharmacologically in vitro and in vivo and resulted in a rapid and robust induction of c‐Jun protein expression. Interestingly, ER‐stressed hepatocytes lacking c‐Jun displayed massive cytoplasmic vacuolization due to ER distension. This phenotype correlated with exacerbated and sustained activation of canonical ER stress signaling pathways. Moreover, sustained ER stress in hepatocytes lacking c‐Jun resulted in increased cell damage and apoptosis. ER stress is also a strong inducer of macroautophagy, a cell‐protective mechanism of self‐degradation of cytoplasmic components and organelles. Interestingly, autophagosome numbers in response to ER stress were reduced in hepatocytes lacking c‐Jun. To further validate these findings, macroautophagy was inhibited chemically in ER‐stressed wildtype hepatocytes, which resulted in cytoplasmic vacuolization and increased cell damage closely resembling the phenotypes observed in c‐Jun‐deficient cells. Conclusion: Our findings indicate that c‐Jun protects hepatocytes against excessive activation of the ER stress response and subsequent cell death and provide evidence that c‐Jun functionally links ER stress responses and macroautophagy. (HEPATOLOGY 2012)</div></front></TEI><affiliations><list><country><li>Allemagne</li><li>Autriche</li></country><region><li>Bade-Wurtemberg</li><li>District de Fribourg-en-Brisgau</li><li>Vienne (Autriche)</li></region><settlement><li>Fribourg-en-Brisgau</li><li>Vienne (Autriche)</li></settlement></list><tree><country name="Allemagne"><region name="Bade-Wurtemberg"><name sortKey="Fuest, Matthias" sort="Fuest, Matthias" uniqKey="Fuest M" first="Matthias" last="Fuest">Matthias Fuest</name></region><name sortKey="Blum, Hubert E" sort="Blum, Hubert E" uniqKey="Blum H" first="Hubert E." last="Blum">Hubert E. Blum</name><name sortKey="Hasselblatt, Peter" sort="Hasselblatt, Peter" uniqKey="Hasselblatt P" first="Peter" last="Hasselblatt">Peter Hasselblatt</name><name sortKey="Hasselblatt, Peter" sort="Hasselblatt, Peter" uniqKey="Hasselblatt P" first="Peter" last="Hasselblatt">Peter Hasselblatt</name><name sortKey="Hasselblatt, Peter" sort="Hasselblatt, Peter" uniqKey="Hasselblatt P" first="Peter" last="Hasselblatt">Peter Hasselblatt</name><name sortKey="Macnelly, Sabine" sort="Macnelly, Sabine" uniqKey="Macnelly S" first="Sabine" last="Macnelly">Sabine Macnelly</name><name sortKey="Willim, Karolina" sort="Willim, Karolina" uniqKey="Willim K" first="Karolina" last="Willim">Karolina Willim</name></country><country name="Autriche"><region name="Vienne (Autriche)"><name sortKey="Fellner, Nicole" sort="Fellner, Nicole" uniqKey="Fellner N" first="Nicole" last="Fellner">Nicole Fellner</name></region><name sortKey="Resch, Guenter P" sort="Resch, Guenter P" uniqKey="Resch G" first="Guenter P." last="Resch">Guenter P. 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