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Contrast-enhanced Magnetic Resonance Imaging of Tumor-bearing Mice Treated with Human Recombinant Tumor Necrosis Factor α

Klaus P. Aicher, Jean W. Dupon, David L. White, Sharon L. Aukerman, Michael E. Moseley, Richard Juster, Werner Rosenau, Jeffrey L. Winkelhake and Robert C. Brasch
Klaus P. Aicher
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Jean W. Dupon
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David L. White
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Sharon L. Aukerman
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Michael E. Moseley
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Richard Juster
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Werner Rosenau
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Jeffrey L. Winkelhake
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Robert C. Brasch
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DOI:  Published November 1990
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Abstract

Pharmacological effects of recombinant human tumor necrosis factor α (TNF) were studied in a mouse fibrosarcoma model using magnetic resonance imaging enhanced with a macromolecular contrast agent, albumin(gadolinium-diethylenetriamine pentaacetic acid)35. TNF was administered i.v. in a dose of 150 µg/kg, 60 to 80 min prior to imaging. Contrast-enhanced and nonenhanced magnetic resonance images of TNF-treated (n = 10) and untreated (n = 8) Meth A fibrosarcomas were obtained at 2.0 Tesla using T1-weighted spin-echo pulse sequences. Serial images spanning an interval of 60 to 120 min after TNF administration showed that the TNF-treated tumors enhanced significantly more overall than did untreated tumors (43% versus 31%). The most marked differential tumor enhancement was observed in the tumor rim (59% versus 40%). Nontumorous tissue, including muscle and brain, revealed no significant enhancement differences between TNF-treated animals and controls. The observed tumor enhancement corresponded strongly with Evans blue staining; the TNF-treated tumors stained deep blue, while untreated tumors and normal tissues observed did not stain. The different enhancement and Evans blue staining patterns between TNF-treated tumors and untreated tumors are attributed to TNF-induced changes in tumor capillary integrity. The data indicate that TNF effects on tumors include an increased capillary permeability for macromolecules at early times after administration. The ability to detect changes in capillary permeability in vivo using contrast-enhanced magnetic resonance imaging may prove to be clinically useful to monitor tumor response to TNF.

Footnotes

  • ↵1 This study was supported, in part, by CA 49786 and DK 31937.

  • ↵2 To whom requests for reprints should be addressed, at Contrast Media Laboratory, Department of Radiology, University of California, San Francisco, 513 Parnassus Avenue, San Francisco, CA 94143-0628.

  • Received May 4, 1990.
  • Accepted August 17, 1990.
  • ©1990 American Association for Cancer Research.
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November 1990
Volume 50, Issue 22
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Contrast-enhanced Magnetic Resonance Imaging of Tumor-bearing Mice Treated with Human Recombinant Tumor Necrosis Factor α
Klaus P. Aicher, Jean W. Dupon, David L. White, Sharon L. Aukerman, Michael E. Moseley, Richard Juster, Werner Rosenau, Jeffrey L. Winkelhake and Robert C. Brasch
Cancer Res November 15 1990 (50) (22) 7376-7381;

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Contrast-enhanced Magnetic Resonance Imaging of Tumor-bearing Mice Treated with Human Recombinant Tumor Necrosis Factor α
Klaus P. Aicher, Jean W. Dupon, David L. White, Sharon L. Aukerman, Michael E. Moseley, Richard Juster, Werner Rosenau, Jeffrey L. Winkelhake and Robert C. Brasch
Cancer Res November 15 1990 (50) (22) 7376-7381;
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