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Experimental Therapeutics

The Use of the l-Plastin Promoter for Adenoviral-mediated, Tumor-specific Gene Expression in Ovarian and Bladder Cancer Cell Lines

Xue Yan Peng, Jong Ho Won, Thomas Rutherford, Takuma Fujii, Daniel Zelterman, Giuseppi Pizzorno, Eva Sapi, John Leavitt, Barry Kacinski, Ronald Crystal, Peter Schwartz and Albert Deisseroth
Xue Yan Peng
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Jong Ho Won
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Thomas Rutherford
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Takuma Fujii
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Daniel Zelterman
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Giuseppi Pizzorno
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Eva Sapi
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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John Leavitt
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Barry Kacinski
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Ronald Crystal
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Peter Schwartz
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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Albert Deisseroth
Genetic Therapy Program, Yale Cancer Center [X. Y. P., J. H. W., T. F., D. Z., G. P., J. L., A. D.], Medical Oncology Section, Departments of Internal Medicine, Therapeutic Radiology Program [E. S., B. K.], and Obstetrics and Gynecology [T. R., P. S.], Yale University School of Medicine, New Haven, Connecticut 06520, and Cornell Medical School, New York, New York, 10021 [R. C.]
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DOI:  Published June 2001
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Abstract

A 2.4-kb truncated l-plastin promoter was inserted either 5′ to the LacZ gene (Ad-Lp-LacZ) or 5′ to the cytosine deaminase (CD) gene (Ad-Lp-CD) in a replication-incompetent adenoviral vector backbone. Infectivity and cytotoxicity experiments with the LacZ and CD vectors suggested that the l-plastin promoter-driven transcriptional units were expressed at much higher levels in explants of ovarian cancer cells from patients and in established ovarian or bladder cancer cell lines than they were in normal peritoneal mesothelial cells from surgical specimens, in organ cultures of normal ovarian cells, or in the established CCD minimal deviation fibroblast cell line. Control experiments showed that this difference was not attributable to the lack of infectivity of the normal peritoneal cells, the normal ovarian cells, or the minimal deviation CCD fibroblast cell line, because these cells showed expression of the LacZ reporter gene when exposed to the replication-incompetent adenoviral vector carrying the cytomegalovirus (CMV)-driven LacZ gene (Ad-CMV-LacZ). The Ovcar-5 and Skov-3 ovarian cancer cell lines exposed to the Ad-Lp-CD adenoviral vector were much more sensitive to the prodrug 5-fluorocytosine (5FC), which is converted from the 5FC prodrug into the toxic chemical 5-fluorouracil, than was the CCD minimal deviation fibroblast cell line after exposure to the same vector. A mouse xenograft model was used to show that the Ad-Lp-CD vector/5FC system could prevent engraftment of ovarian cancer cells in nude mice. Finally, injection of the Ad-Lp-CD vector into s.c. tumor nodules generated a greater reduction of the size of the tumor nodules than did injection of the Ad-CMV-LacZ vectors into tumor nodules. The Ad-Lp-CD vectors were as suppressive to tumor growth as the Ad-CMV-CD vectors. These results suggest that an adenoviral vector carrying the CD gene controlled by the l-plastin promoter (Ad-Lp-CD) may be of potential value for the i.p. therapy of ovarian cancer.

  • Received February 3, 2000.
  • Accepted April 10, 2001.
  • ©2001 American Association for Cancer Research.
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Cancer Research: 61 (11)
June 2001
Volume 61, Issue 11
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The Use of the l-Plastin Promoter for Adenoviral-mediated, Tumor-specific Gene Expression in Ovarian and Bladder Cancer Cell Lines
Xue Yan Peng, Jong Ho Won, Thomas Rutherford, Takuma Fujii, Daniel Zelterman, Giuseppi Pizzorno, Eva Sapi, John Leavitt, Barry Kacinski, Ronald Crystal, Peter Schwartz and Albert Deisseroth
Cancer Res June 1 2001 (61) (11) 4405-4413;

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The Use of the l-Plastin Promoter for Adenoviral-mediated, Tumor-specific Gene Expression in Ovarian and Bladder Cancer Cell Lines
Xue Yan Peng, Jong Ho Won, Thomas Rutherford, Takuma Fujii, Daniel Zelterman, Giuseppi Pizzorno, Eva Sapi, John Leavitt, Barry Kacinski, Ronald Crystal, Peter Schwartz and Albert Deisseroth
Cancer Res June 1 2001 (61) (11) 4405-4413;
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