Literature DB >> 8760114

Inhibition of binding to fatty acid binding protein reduces the intracellular transport of fatty acids.

B A Luxon1.   

Abstract

Male livers, containing lesser amounts of fatty acid binding protein (FABP), utilize fatty acids more slowly than female livers. Conventional wisdom dictates that FABP stimulates fatty acid use by increasing cytoplasmic transport rates. Previously, we showed that the cytoplasmic diffusion of a fatty acid analogue [12-N-methyl-7-nitrobenzo-2-oxa-1,3-diazol-amino stearate (NBD-stearate)] is faster in female hepatocytes, paralleling the larger amounts of FABP. Sex differences in other cytoplasmic factors could also lead to faster diffusion, independent of FABP levels. The aim of this study was to determine the effect of inhibition of fatty acid binding to FABP on the directly measured intracellular transport rate of NBD-stearate. The binding of NBD-stearate to FABP was reduced by incubating hepatocytes isolated from male and female rats with alpha-bromo-palmitate (0-1,500 microM), a modified long-chain fatty acid that binds to FABP. The inhibition by alpha-bromo-palmitate on NBD-stearate binding to FABP was measured with the use of centrifugation to separate cytosol from cytoplasmic membranes. Laser photobleaching (fluorescence recovery after photobleaching) was used to measure the cytoplasmic diffusion of NBD-stearate in hepatocytes. Alpha-Bromo-palmitate incubation reduced NBD-stearate binding to FABP in a dose-dependent manner. The measured diffusion rate was also reduced in proportion to the degree of binding inhibition. We conclude that cytoplasmic transport of NBD-stearate is modulated by binding to soluble proteins like FABP. FABP enhances diffusive transport by reducing binding to immobile cytosolic membranes.

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Year:  1996        PMID: 8760114     DOI: 10.1152/ajpgi.1996.271.1.G113

Source DB:  PubMed          Journal:  Am J Physiol        ISSN: 0002-9513


  10 in total

1.  Cellular pharmacokinetics: effects of cytoplasmic diffusion and binding on organ transit time distribution.

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Journal:  J Pharmacokinet Biopharm       Date:  1999-06

Review 2.  Cytosolic fatty acid binding proteins catalyze two distinct steps in intracellular transport of their ligands.

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3.  Cytoplasmic binding and disposition kinetics of diclofenac in the isolated perfused rat liver.

Authors:  M Weiss; O Kuhlmann; D Y Hung; M S Roberts
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4.  Assessing the cellular transmembrane electrical potential difference on the hepatic uptake of palmitate.

Authors:  F J Burczynski; D Hung; G Q Wang; B Elmadhoun; A Lewis; P Chang; G Rajaraman; S Robert
Journal:  Mol Cell Biochem       Date:  2005-02       Impact factor: 3.396

5.  Membrane binding proteins are the major determinants for the hepatocellular transmembrane flux of long-chain fatty acids bound to albumin.

Authors:  G Rajaraman; M S Roberts; D Hung; G Q Wang; F J Burczynski
Journal:  Pharm Res       Date:  2005-08-16       Impact factor: 4.200

6.  Fatty acid binding proteins: potential chaperones of cytosolic drug transport in the enterocyte?

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Review 7.  Pathways of polyunsaturated fatty acid utilization: implications for brain function in neuropsychiatric health and disease.

Authors:  Joanne J Liu; Pnina Green; J John Mann; Stanley I Rapoport; M Elizabeth Sublette
Journal:  Brain Res       Date:  2014-12-08       Impact factor: 3.252

8.  Beta-glucan extracts inhibit the in vitro intestinal uptake of long-chain fatty acids and cholesterol and down-regulate genes involved in lipogenesis and lipid transport in rats.

Authors:  Laurie A Drozdowski; Raylene A Reimer; Feral Temelli; Rhonda C Bell; Thava Vasanthan; Alan B R Thomson
Journal:  J Nutr Biochem       Date:  2009-08-27       Impact factor: 6.048

9.  Molecular mechanism of recombinant liver fatty acid binding protein's antioxidant activity.

Authors:  Jing Yan; Yuewen Gong; Yi-Min She; Guqi Wang; Michael S Roberts; Frank J Burczynski
Journal:  J Lipid Res       Date:  2009-05-27       Impact factor: 5.922

10.  Fabp7 maps to a quantitative trait locus for a schizophrenia endophenotype.

Authors:  Akiko Watanabe; Tomoko Toyota; Yuji Owada; Takeshi Hayashi; Yoshimi Iwayama; Miho Matsumata; Yuichi Ishitsuka; Akihiro Nakaya; Motoko Maekawa; Tetsuo Ohnishi; Ryoichi Arai; Katsuyasu Sakurai; Kazuo Yamada; Hisatake Kondo; Kenji Hashimoto; Noriko Osumi; Takeo Yoshikawa
Journal:  PLoS Biol       Date:  2007-11       Impact factor: 8.029

  10 in total

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