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Research ArticleArticle

Absorption Enhancement, Structural Changes in Tight Junctions and Cytotoxicity Caused by Palmitoyl Carnitine in Caco-2 and IEC-18 Cells

Erwin Duizer, Cees Van Der Wulp, Carolien H. M. Versantvoort and John P. Groten
Journal of Pharmacology and Experimental Therapeutics October 1998, 287 (1) 395-402;
Erwin Duizer
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Cees Van Der Wulp
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Carolien H. M. Versantvoort
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John P. Groten
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Abstract

Palmitoyl carnitine chloride (PCC) has been shown to be an effective enhancer of intestinal transport of hydrophilic molecules. The exact mechanism by which the epithelial barrier function is decreased is not clear. In an attempt to elucidate the mechanism of action of PCC, we studied the relationship among absorption enhancement, cell viability and tight junction protein localization in the human colonic Caco-2 cell line and the rat small intestinal cell line IEC-18. Filter-grown cells were exposed to 0 to 1 mM PCC for 30 min, and the efficacy of PCC treatment was determined by assessing the transepithelial electrical resistance and the apparent permeability for mannitol and PEG-4000. Membrane lysis and cytotoxicity were assessed by measurement of lactate dehydrogenase leakage and uptake of propidium iodide and neutral red. The immunolocalization of the tight junctional protein ZO-1 was quantified using CSLM and image-processing software. In both cell lines, PCC caused a dose-dependent decrease in transepithelial electrical resistance and a concomitant increase in the permeability for mannitol and PEG-4000. The transport enhancement was accompanied by an increase in apical membrane permeability and a reduction in cell viability. At higher PCC concentrations (≥0.4 mM), the distribution of the tight junctional protein ZO-1 was changed and cells were unable to recover viability. PCC is effective as an absorption enhancer for hydrophilic macromolecules. However, lytic effects on the cell membrane and reduced cell viability were concomitant with transport enhancement.

Footnotes

  • Send reprint requests to: Dr. Erwin Duizer, TNO Nutrition and Food Research Institute, Toxicology Division, P.O. Box 360, 3700 AJ Zeist, Netherlands.

  • ↵1 Present address: TNO Prince Maurits Laboratory, Rijswijk, Netherlands

  • Abbreviations:
    PCC
    palmitoyl carnitine chloride
    PEG
    polyethylene glycol
    CSLM
    confocal scanning laser microscopy
    FCS
    fetal calf serum
    TER
    transepithelial electrical resistance
    DMEM
    Dulbecco’s modified Eagle’s medium
    HBSS
    Hank’s balanced salt solution
    LDH
    lactate dehydrogenase
    PI
    propidium iodide
    NR
    neutral red
    • Received September 25, 1997.
    • Accepted May 19, 1998.
  • The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics
Vol. 287, Issue 1
1 Oct 1998
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Research ArticleArticle

Absorption Enhancement, Structural Changes in Tight Junctions and Cytotoxicity Caused by Palmitoyl Carnitine in Caco-2 and IEC-18 Cells

Erwin Duizer, Cees Van Der Wulp, Carolien H. M. Versantvoort and John P. Groten
Journal of Pharmacology and Experimental Therapeutics October 1, 1998, 287 (1) 395-402;

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Research ArticleArticle

Absorption Enhancement, Structural Changes in Tight Junctions and Cytotoxicity Caused by Palmitoyl Carnitine in Caco-2 and IEC-18 Cells

Erwin Duizer, Cees Van Der Wulp, Carolien H. M. Versantvoort and John P. Groten
Journal of Pharmacology and Experimental Therapeutics October 1, 1998, 287 (1) 395-402;
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