In vivo antitumor activity of S16020, a topoisomerase II inhibitor, and doxorubicin against human brain tumor xenografts

Gilles Vassal; Jean-Louis Merlin; Marie-José Terrier-Lacombe; Jacques Grill; Fabrice Parker; Christian Sainte-Rose; Geneviève Aubert; Jackie Morizet; Nicolas Sévenet; Marie-Gwenaëlle Poullain; Catherine Lucas; Chantal Kalifa

doi:10.1007/s00280-003-0584-1

In vivo antitumor activity of S16020, a topoisomerase II inhibitor, and doxorubicin against human brain tumor xenografts

Cancer Chemother Pharmacol. 2003 May;51(5):385-94. doi: 10.1007/s00280-003-0584-1. Epub 2003 Mar 22.

Authors

Gilles Vassal¹, Jean-Louis Merlin, Marie-José Terrier-Lacombe, Jacques Grill, Fabrice Parker, Christian Sainte-Rose, Geneviève Aubert, Jackie Morizet, Nicolas Sévenet, Marie-Gwenaëlle Poullain, Catherine Lucas, Chantal Kalifa

Affiliation

¹ UPRES EA 3535 Pharmacology and New Treatments of Cancers, Institut Gustave-Roussy, Villejuif, France. gvassal@igr.fr

PMID: 12736760
DOI: 10.1007/s00280-003-0584-1

Abstract

New active drugs are needed for the treatment of primary brain tumors in both children and adults. S16020 is a cytotoxic olivacine derivative that inhibits topoisomerase II. The aim of the study was to determine its antitumor activity in athymic mice bearing subcutaneous medulloblastoma (IGRM33, 34, 57) and glioblastoma (IGRG88, 93, 121) xenografts treated at an advanced stage of tumor growth in comparison with that of doxorubicin. Animals were randomly assigned to receive i.v. S16020 or doxorubicin weekly for three consecutive weeks. The optimal dose was 80 mg/kg per week. S16020 demonstrated a significant antitumor activity in two out of three medulloblastoma xenografts. IGRM57 xenografts were highly sensitive with 100% tumor regressions and a tumor growth delay (TGD) of 102 days, while one of eight IGRM34 xenografts showed a partial regression with a TGD of 16 days. Doxorubicin was significantly more active than S16020 in these two models. IGRM33, a model established from a tumor in relapse after chemotherapy and radiotherapy, was refractory to both drugs. S16020 demonstrated a significant antitumor activity in the three glioblastoma xenografts evaluated. The wild-type p53 IGRG93 xenograft was highly sensitive with 100% tumor regressions and a TGD of 54 days. IGRG121 (wt p53) and IGRG88 (mutant p53) were moderately sensitive with TGDs of 33 and 23 days, respectively. Doxorubicin showed greater activity in two of these models. All six xenografts exhibited low expression of mdr1 as quantitated by RT-PCR, and no correlation was found with the activity of either drug. Conversely, a low activity of the two drugs was significantly associated with a high expression of MRP1 in medulloblastomas. Finally, no relationship was observed between drug sensitivity to either drug and expression of their target, topoisomerase IIalpha. In conclusion, S16020 and doxorubicin showed significant antitumor activity in brain tumor xenografts treated at an advanced stage of tumor growth. Their activity was related to MRP1 expression in medulloblastomas.

MeSH terms

Animals
Carbazoles / pharmacology*
Cerebellar Neoplasms / drug therapy*
Cerebellar Neoplasms / pathology
Cerebellar Neoplasms / veterinary
Doxorubicin / pharmacology*
Drug Therapy, Combination
Female
Gene Expression Regulation
Glioblastoma / drug therapy*
Glioblastoma / pathology
Glioblastoma / veterinary
Medulloblastoma / drug therapy*
Medulloblastoma / pathology
Medulloblastoma / veterinary
Mice
Mice, Nude
Multidrug Resistance-Associated Proteins / biosynthesis*
Multidrug Resistance-Associated Proteins / pharmacology
Pyridines / pharmacology*
Reverse Transcriptase Polymerase Chain Reaction
Topoisomerase II Inhibitors*
Transplantation, Heterologous

Substances

Carbazoles
Multidrug Resistance-Associated Proteins
NSC 659687
Pyridines
Topoisomerase II Inhibitors
Doxorubicin
multidrug resistance-associated protein 1