Literature DB >> 28835543

Zonation of hepatic fat accumulation: insights from mathematical modelling of nutrient gradients and fatty acid uptake.

Jana Schleicher1,2, Uta Dahmen3, Reinhard Guthke4, Stefan Schuster2.   

Abstract

Intrinsic of non-alcoholic fatty liver diseases is an aberrant accumulation of triglycerides (steatosis), which occurs inhomogeneously within lobules. To improve our understanding of the mechanisms involved in this zonation patterning, we developed a mathematical multicompartment model of hepatic fatty acid metabolism accompanied by blood flow simulations. A model analysis determines the influence of the uptake process of fatty acids, the porto-central gradient of plasma fatty acid concentration, and the oxygen supply via blood on the zonation of triglyceride accumulation. From this theoretical perspective, the plasma oxygen gradient, but not the fatty acid gradient, leads the way to a zonated triglyceride accumulation by its decisive role in oxidative processes. In addition, the uptake mechanism of fatty acids seems to be fundamental for a pericentral dominance of steatosis. However, the mechanism of cellular fatty acid uptake from the blood is still under debate. Our theoretical approach supports the transporter-mediated uptake mechanism and reveals that the maximal velocity of fatty acid uptake affects the switching between a periportal and a pericentral triglyceride accumulation. Further research on hepatic fatty acid uptake is needed to push forward our understanding of aberrant triglyceride accumulation in diet-induced steatosis.
© 2017 The Author(s).

Entities:  

Keywords:  fatty acid uptake; liver metabolism; metabolic zonation; non-alcoholic fatty liver diseases; steatosis

Mesh:

Substances:

Year:  2017        PMID: 28835543      PMCID: PMC5582132          DOI: 10.1098/rsif.2017.0443

Source DB:  PubMed          Journal:  J R Soc Interface        ISSN: 1742-5662            Impact factor:   4.118


  101 in total

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2.  Short-term inhibition of SREBP-1c expression reverses diet-induced non-alcoholic fatty liver disease in mice.

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7.  Computational experiments reveal plausible mechanisms for changing patterns of hepatic zonation of xenobiotic clearance and hepatotoxicity.

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8.  Nonalcoholic steatohepatitis: a proposal for grading and staging the histological lesions.

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2.  A microfluidic patterned model of non-alcoholic fatty liver disease: applications to disease progression and zonation.

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4.  A multiscale modelling approach to assess the impact of metabolic zonation and microperfusion on the hepatic carbohydrate metabolism.

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5.  Modeling of xenobiotic transport and metabolism in virtual hepatic lobule models.

Authors:  Xiao Fu; James P Sluka; Sherry G Clendenon; Kenneth W Dunn; Zemin Wang; James E Klaunig; James A Glazier
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6.  Normothermic Ex Vivo Liver Platform Using Porcine Slaughterhouse Livers for Disease Modeling.

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Review 7.  Computational Modeling in Liver Surgery.

Authors:  Bruno Christ; Uta Dahmen; Karl-Heinz Herrmann; Matthias König; Jürgen R Reichenbach; Tim Ricken; Jana Schleicher; Lars Ole Schwen; Sebastian Vlaic; Navina Waschinsky
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9.  Computational Modeling of Oxidative Stress in Fatty Livers Elucidates the Underlying Mechanism of the Increased Susceptibility to Ischemia/Reperfusion Injury.

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10.  Biocompatibility studies of fluorescent diamond particles-(NV)~800nm (part V): in vitro kinetics and in vivo localization in rat liver following long-term exposure.

Authors:  Jonathan A Gerstenhaber; Cezary Marcinkiewicz; Frank C Barone; Mark Sternberg; Michael R D'Andrea; Peter I Lelkes; Giora Z Feuerstein
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  10 in total

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