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Experimental Therapeutics, Molecular Targets, and Chemical Biology

BN80927

A Novel Homocamptothecin That Inhibits Proliferation of Human Tumor Cells in Vitro and in Vivo

Danièle Demarquay, Marion Huchet, Helène Coulomb, Laurence Lesueur-Ginot, Olivier Lavergne, José Camara, Philip G. Kasprzyk, Grégoire Prévost and Dennis C. H. Bigg
Danièle Demarquay
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Marion Huchet
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Helène Coulomb
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Laurence Lesueur-Ginot
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Olivier Lavergne
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José Camara
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Philip G. Kasprzyk
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Grégoire Prévost
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Dennis C. H. Bigg
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DOI: 10.1158/0008-5472.CAN-03-3872 Published July 2004
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Abstract

BN80927 belongs to a novel family of camptothecin analogs, the homocamptothecins, developed on the concept of topoisomerase I (Topo I) inhibition and characterized by a stable seven-membered β-hydroxylactone ring. Preclinical data reported here show that BN80927 retains Topo I poisoning activity in cell-free assay (DNA relaxation) as well as in living cells, in which in vivo complexes of topoisomerase experiments and quantification of DNA-protein-complexes stabilization, have confirmed the higher potency of BN80927 as compared with the Topo I inhibitor SN38. In addition, BN80927 inhibits Topo II-mediated DNA relaxation in vitro but without cleavable-complex stabilization, thus indicating catalytic inhibition. Moreover, a Topo I-altered cell line (KBSTP2), resistant to SN38, remains sensitive to BN80927, suggesting that a part of the antiproliferative effects of BN80927 are mediated by a Topo I-independent pathway. This hypothesis is also supported by in vitro data showing an antiproliferative activity of BN80927 on a model of resistance related to the noncycling state of cells (G0-G1 synchronized). In cell growth assays, BN80927 is a very potent antiproliferative agent as shown by IC50 values consistently lower than those of SN38 in tumor cell lines as well as in their related drug-resistant lines. BN80927 shows high efficiency in vivo in tumor xenograft studies using human androgen-independent prostate tumors PC3 and DU145. Altogether, these data strongly support the clinical development of BN80927.

Footnotes

  • The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked advertisement in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

  • Requests for reprints: Danièle Demarquay, Institut Henri Beaufour, 5, avenue du Canada, F-91966 Les Ulis, France. Phone: 33-1-60-92-20-00; Fax: 33-1-69-07-38-02; E-mail: daniele.demarquay{at}ipsen.com

  • Received December 11, 2003.
  • Revision received February 18, 2004.
  • Accepted May 6, 2004.
  • ©2004 American Association for Cancer Research.
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Cancer Research: 64 (14)
July 2004
Volume 64, Issue 14
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BN80927
Danièle Demarquay, Marion Huchet, Helène Coulomb, Laurence Lesueur-Ginot, Olivier Lavergne, José Camara, Philip G. Kasprzyk, Grégoire Prévost and Dennis C. H. Bigg
Cancer Res July 15 2004 (64) (14) 4942-4949; DOI: 10.1158/0008-5472.CAN-03-3872

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BN80927
Danièle Demarquay, Marion Huchet, Helène Coulomb, Laurence Lesueur-Ginot, Olivier Lavergne, José Camara, Philip G. Kasprzyk, Grégoire Prévost and Dennis C. H. Bigg
Cancer Res July 15 2004 (64) (14) 4942-4949; DOI: 10.1158/0008-5472.CAN-03-3872
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