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63 research outputs found

Preclinical antitumour activity of F 11782, a novel dual catalytic inhibitor of topoisomerases

Author: Colpaert F
Etiévant C
Hill B T
Imbert T
Kruczynski A
Perrin D
Publication venue: Nature Publishing Group
Publication date
Field of study

F 11782 is a novel inhibitor of topoisomerases I and II, with an original mechanism of action (Perrin et al, 2000). This study, aimed to define its anticancer efficacy against a series of murine and human tumour models, has provided evidence of major antitumour activity for F 11782. This was demonstrated as a high level of activity against the P388 leukaemia, as reflected by increased survival of 143–457%, when administered i.p., p.o. or i.v. as single or multiple doses, and proved consistently superior to etoposide or camptothecin tested concurrently. Single or multiple i.p. doses of F 11782 also proved highly active against the s.c. grafted B16 melanoma, significantly increasing survival (P < 0.001) and inhibiting tumour growth (T/C of 0.3%), again superior to etoposide tested concurrently. Furthermore, F 11782 inhibited the number of pulmonary metastatic foci of the B16F10 melanoma by 99%. In human tumour xenograft studies, multiple i.p. doses of F 11782 resulted in major inhibitory activity against MX-1 (breast) tumours (T/C of 0.1%), as well as causing definite tumour regressions, whereas none resulted from similar experimental treatments with etoposide. Significant activity was also recorded with F 11782 against the relatively refractory LX-1 (lung) xenografts, with an optimal T/C value of 19%. It was notable that the antitumour activity of F 11782 was consistently demonstrated over a wide range of 2–6 dose levels, providing evidence of its good overall tolerance. In conclusion, these results emphasize the preclinical interest of this novel molecule and support its further preclinical development. © 2000 Cancer Research Campaign http://www.bjcancer.co

Crossref

PubMed Central

Characterization of cell death induced by vinflunine, the most recent Vinca alkaloid in clinical development

Author: A Basu
A Duflos
A Kruczynski
A Kruczynski
A Kruczynski
AA Stone
AH Wyllie
B T Hill
BA Rupnow
BT Hill
C Etiévant
C Etiévant
CY Wang
D Hockenbery
D Perrin
DK Miller
H Zhang
HC Toh
J Fahy
JM Brown
K Torres
LG Wang
MT Osborn
N Chansard
N Fujita
OJ Stoetzer
P Fumoleau
Q Cheng
R Bertrand
RK Srivastava
RU Jänicke
S Haldar
S Haldar
S Lobert
SC Kaufmann
SC Lowe
SL Mooberry
T-H Wang
UA Germann
Publication venue: Nature Publishing Group
Publication date
Field of study

Vinflunine, the most recent Vinca alkaloid in clinical development, demonstrated superior antitumour activity to other Vincas in preclinical tumour models. This study aimed to define its molecular mechanisms of cell killing in both parental sensitive and vinflunine-resistant P388 leukaemia cells. Vinflunine treatment of these cells resulted in apoptosis characterized by DNA fragmentation and proteolytic cleavage of poly-(ADP-ribose) polymerase. Apoptosis-inducing concentrations of vinflunine caused c-Jun N-terminal kinase 1 stimulation, as well as caspases-3/7 activation. This activation of caspases and the induction of apoptosis could be inhibited by the caspase inhibitor acetyl-Asp-Glu-Val-Asp-aldehyde. Interestingly, the apoptosis signal triggered by vinflunine in these P388 cells was not mediated through Bcl-2 phosphorylation. In addition, when vinflunine resistance was developed in P388 cells, it was associated with resistance to vinflunine-induced apoptosis, as reflected by a loss of capacity to induce DNA fragmentation and PARP degradation, and characterized by increased levels of Bcl-2 and Bfl-1/A1. Therefore, these data indirectly implicate Bcl-2 and Bfl-1/A1 in vinflunine-induced cell death mechanisms

Crossref

PubMed Central