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Research ArticleCHEMOTHERAPY, ANTIBIOTICS, AND GENE THERAPY

Intracellular Localization of the Radiation Enhancer Motexafin Gadolinium Using Interferometric Fourier Fluorescence Microscopy

Kathryn W. Woodburn
Journal of Pharmacology and Experimental Therapeutics June 2001, 297 (3) 888-894;
Kathryn W. Woodburn
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Abstract

Motexafin gadolinium (MGd) is a unique therapeutic agent that localizes in cancer cells and increases tumor response to ionizing radiation and certain chemotherapeutics. The in vitro intracellular localization, accumulation, and retention of MGd in murine EMT6 mammary sarcoma and Rif-1 fibrosarcoma cell lines were studied using interferometric Fourier fluorescence microscopy. MGd cellular uptake was semiquantified using its characteristic fluorescence emission band centered at 758 nm. Colocalization studies were performed using mitochondrial, endoplasmic reticulum, Golgi apparatus, nuclear, and lysosomal fluorescent organelle probes, and verified using interferometric Fourier spectroscopy. Cellular uptake was gradual and increased significantly with incubation time. MGd localized primarily within the lysosomes and endoplasmic reticulum, and to a lesser extent within the Golgi apparatus and mitochondria. Mitochondrial staining was increased in media without serum. No nuclear uptake was detected in the Rif-1 cells, but after 48 h nuclear uptake was observed in 15% of EMT6 cells. These results indicated that MGd accumulates within cytoplasmic compartments. The sustained intracellular localization of MGd may, in part, account for its unique radiation and chemotherapy enhancement properties. Interferometric Fourier fluorescence microscopy is a potentially powerful tool in delineating and verifying localization sites of therapeutic agents.

Footnotes

  • Send reprint requests to: Kathryn W. Woodburn, Ph.D., Pharmacyclics, 995 East Arques Ave., Sunnyvale, CA 94086. E-mail:KWoodburn{at}pcyc.com

  • Abbreviations:
    MGd
    motexafin gadolinium
    MTG
    MitoTracker Green FM
    LTR
    LysoTracker red DND-99
    C5-ceramide
    BODIPY FL C5-ceramide
    R6
    Rhodamine B, hexyl ester, perchlorate
    HO342
    Hoechst 33342
    FBS
    fetal bovine serum
    CCD
    charge-coupled device
    FWHM
    full-width half-maximum
    • Received October 20, 2000.
    • Accepted February 20, 2001.
  • The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics: 297 (3)
Journal of Pharmacology and Experimental Therapeutics
Vol. 297, Issue 3
1 Jun 2001
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Research ArticleCHEMOTHERAPY, ANTIBIOTICS, AND GENE THERAPY

Intracellular Localization of the Radiation Enhancer Motexafin Gadolinium Using Interferometric Fourier Fluorescence Microscopy

Kathryn W. Woodburn
Journal of Pharmacology and Experimental Therapeutics June 1, 2001, 297 (3) 888-894;

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Research ArticleCHEMOTHERAPY, ANTIBIOTICS, AND GENE THERAPY

Intracellular Localization of the Radiation Enhancer Motexafin Gadolinium Using Interferometric Fourier Fluorescence Microscopy

Kathryn W. Woodburn
Journal of Pharmacology and Experimental Therapeutics June 1, 2001, 297 (3) 888-894;
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