Literature DB >> 23926289

Olanzapine activates hepatic mammalian target of rapamycin: new mechanistic insight into metabolic dysregulation with atypical antipsychotic drugs.

Robin H Schmidt1, Jenny D Jokinen, Veronica L Massey, K Cameron Falkner, Xue Shi, Xinmin Yin, Xiang Zhang, Juliane I Beier, Gavin E Arteel.   

Abstract

Olanzapine (OLZ), an effective treatment of schizophrenia and other disorders, causes weight gain and metabolic syndrome. Most studies to date have focused on the potential effects of OLZ on the central nervous system's mediation of weight; however, peripheral changes in liver or other key metabolic organs may also play a role in the systemic effects of OLZ. Thus, the purpose of this study was to investigate the effects of OLZ on hepatic metabolism in a mouse model of OLZ exposure. Female C57Bl/6J mice were administered OLZ (8 mg/kg per day) or vehicle subcutaneously by osmotic minipumps for 28 days. Liver and plasma were taken at sacrifice for biochemical analyses and for comprehensive two-dimensional gas chromatography coupled to time-of-flight mass spectrometry metabolomics analysis. OLZ increased body weight, fat pad mass, and liver-to-body weight ratio without commensurate increase in food consumption, indicating that OLZ altered energy expenditure. Expression and biochemical analyses indicated that OLZ induced anaerobic glycolysis and caused a pseudo-fasted state, which depleted hepatic glycogen reserves. OLZ caused similar effects in cultured HepG2 cells, as determined by Seahorse analysis. Metabolomic analysis indicated that OLZ increased hepatic concentrations of amino acids that can alter metabolism via the mTOR pathway; indeed, hepatic mTOR signaling was robustly increased by OLZ. Interestingly, OLZ concomitantly activated AMP-activated protein kinase (AMPK) signaling. Taken together, these data suggest that disturbances in glucose and lipid metabolism caused by OLZ in liver may be mediated, at least in part, via simultaneous activation of both catabolic (AMPK) and anabolic (mammalian target of rapamycin) pathways, which yields new insight into the metabolic side effects of this drug.

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Year:  2013        PMID: 23926289      PMCID: PMC3781405          DOI: 10.1124/jpet.113.207621

Source DB:  PubMed          Journal:  J Pharmacol Exp Ther        ISSN: 0022-3565            Impact factor:   4.030


  49 in total

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Authors:  Sangwon F Kim; Alex S Huang; Adele M Snowman; Cory Teuscher; Solomon H Snyder
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Review 3.  Atypical antipsychotics: new drugs, new challenges.

Authors:  Manu Mathews; David J Muzina
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Review 4.  Targeting mammalian target of rapamycin (mTOR) for health and diseases.

Authors:  Chi Kwan Tsang; Haiyan Qi; Leroy F Liu; X F Steven Zheng
Journal:  Drug Discov Today       Date:  2006-12-15       Impact factor: 7.851

5.  Hepatic histology in obese patients undergoing bariatric surgery.

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Authors:  Cynthia L Ogden; Margaret D Carroll; Lester R Curtin; Margaret A McDowell; Carolyn J Tabak; Katherine M Flegal
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Review 8.  Interaction between the AMP-activated protein kinase and mTOR signaling pathways.

Authors:  Scot R Kimball
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Authors:  Lisa D Marroquin; James Hynes; James A Dykens; Joseph D Jamieson; Yvonne Will
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  24 in total

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2.  Olanzapine-induced liver injury in mice: aggravation by high-fat diet and protection with sulforaphane.

Authors:  Robin H Isaacson; Juliane I Beier; Nicholas Kh Khoo; Bruce A Freeman; Zachary Freyberg; Gavin E Arteel
Journal:  J Nutr Biochem       Date:  2020-04-08       Impact factor: 6.048

3.  Network analysis of gene expression in peripheral blood identifies mTOR and NF-κB pathways involved in antipsychotic-induced extrapyramidal symptoms.

Authors:  S Mas; P Gassó; E Parellada; M Bernardo; A Lafuente
Journal:  Pharmacogenomics J       Date:  2015-01-27       Impact factor: 3.550

4.  Network analysis of gene expression in mice provides new evidence of involvement of the mTOR pathway in antipsychotic-induced extrapyramidal symptoms.

Authors:  S Mas; P Gassó; D Boloc; N Rodriguez; F Mármol; J Sánchez; M Bernardo; A Lafuente
Journal:  Pharmacogenomics J       Date:  2015-06-30       Impact factor: 3.550

5.  Vinyl Chloride Metabolites Potentiate Inflammatory Liver Injury Caused by LPS in Mice.

Authors:  Lisanne C Anders; Anna L Lang; Anwar Anwar-Mohamed; Amanda N Douglas; Adrienne M Bushau; Keith Cameron Falkner; Bradford G Hill; Nikole L Warner; Gavin E Arteel; Matt Cave; Craig J McClain; Juliane I Beier
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6.  Comparison of GC-MS and GC×GC-MS in the analysis of human serum samples for biomarker discovery.

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Journal:  J Proteome Res       Date:  2015-03-16       Impact factor: 4.466

7.  Autophagy inhibition uncovers the neurotoxic action of the antipsychotic drug olanzapine.

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Journal:  Autophagy       Date:  2014       Impact factor: 16.016

8.  Normal-Gamma-Bernoulli Peak Detection for Analysis of Comprehensive Two-Dimensional Gas Chromatography Mass Spectrometry Data.

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9.  Safety Assessment of Liver Injury with Quetiapine Fumarate XR Management in Very Heavy Drinking Alcohol-Dependent Patients.

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10.  Rapamycin attenuates liver injury caused by vinyl chloride metabolite chloroethanol and lipopolysaccharide in mice.

Authors:  Anna L Lang; Austin M Krueger; Regina D Schnegelberger; Brenna R Kaelin; Maxwell J Rakutt; Liya Chen; Gavin E Arteel; Juliane I Beier
Journal:  Toxicol Appl Pharmacol       Date:  2019-09-06       Impact factor: 4.219

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