DNA interstrand cross-linking and in vivo antitumor activity of the extended pyrrolo[2,1-c][1,4]benzodiazepine dimer SG2057

被引:0
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作者
John A. Hartley
Anzu Hamaguchi
Marie Suggitt
Stephen J. Gregson
David E. Thurston
Philip W. Howard
机构
[1] Spirogen Ltd,
[2] UCL Cancer Institute,undefined
[3] CR-UK Drug-DNA Interactions Research Group,undefined
[4] UCL Cancer Institute,undefined
[5] Spirogen Ltd,undefined
[6] The School of Pharmacy,undefined
[7] University of London,undefined
[8] UCL Cancer Institute,undefined
[9] University College London,undefined
来源
Investigational New Drugs | 2012年 / 30卷
关键词
Pyrrolobenzodiazepine dimer; SG2057; DNA interstrand cross-linking; DNA minor groove binding agent;
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摘要
The pyrrolobenzodiazepines (PBDs) are naturally occurring antitumor antibiotics and a PBD dimer (SJG-136, SG2000) is in Phase II trials. SG2000 is a propyldioxy linked PBD dimer which binds sequence selectively in the minor groove of DNA forming DNA interstrand and intrastrand cross-linked adducts, and also mono-adducts depending on sequence. SG2057 is the corresponding dimer containing a pentyldioxy linkage. SG2057 has multilog differential in vitro cytotoxicity against a panel of human tumour cell lines with a mean GI50 of 212 pM. The agent is highly efficient at producing DNA interstrand cross-links in cells which form rapidly and persist over a 48 h period. Significant antitumor activity was demonstrated in several human tumor xenograft models. Cures were obtained in a LOX-IMVI melanoma model following a single administration and dose-dependent activity, including regression responses, observed in SKOV-3 ovarian and HL-60 promyelocytic leukemia models following repeat dose schedules. In the advanced stage LS174T model, SG2057 administered either as a single dose, or in two repeat dose schedules, was superior to irinotecan. SG2057 is therefore a highly active antitumor agent, with more potent in vitro activity and superior in vivo activity to SG2000, warranting further development.
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页码:950 / 958
页数:8
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