Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles

Topoisomerase I is an enzyme that is essential for maintaining the three-dimensional structure of DNA during the processes of transcription, translation and mitosis. With the introduction of new clinical agents that are effective in poisoning topoisomerase I, this enzyme has proved to be an attracti...

Full description

Saved in:
Bibliographic Details
Main Authors: Rangarajan, M., Kim, J.S., Sim, S.P, Liu, A., Liu, L.F., LaVoie, E.J.
Format: E-Article
Language:English
Published: Bioorganic & Medicinal Chemistry Letters 2000
Subjects:
Online Access:http://ir.unimas.my/id/eprint/2497/1/Topoisomerase%20I%20inhibition%20and%20cytotoxicity%20of%205-Bromo-%20and%205-Phenylterbenzimidazoles.pdf
http://ir.unimas.my/id/eprint/2497/
Tags: Add Tag
No Tags, Be the first to tag this record!
Institution: Universiti Malaysia Sarawak
Language: English
id my.unimas.ir.2497
record_format eprints
spelling my.unimas.ir.24972015-03-20T08:02:55Z http://ir.unimas.my/id/eprint/2497/ Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles Rangarajan, M. Kim, J.S. Sim, S.P Liu, A. Liu, L.F. LaVoie, E.J. QD Chemistry R Medicine (General) Topoisomerase I is an enzyme that is essential for maintaining the three-dimensional structure of DNA during the processes of transcription, translation and mitosis. With the introduction of new clinical agents that are effective in poisoning topoisomerase I, this enzyme has proved to be an attractive molecular target in the development of anticancer drugs. Several terbenzimidazoles have been identified as potent topoisomerase I poisons. Structure–activity data on various terbenzimidazoles have revealed that the presence of lipophilic substituents at the 5-position of various terbenzimidazoles correlates with enhanced cytotoxicity. While the effect of having substituents at both the 5- and 6-positions had not been evaluated, previous studies did indicate that the presence of a fused benzo-ring at the 5,6-position results in a significant decrease in topoisomerase I poisoning activity and cytotoxicity. In the present study we investigated whether substituents at both the 5- and 6-positions of varied terbenzimidazoles would allow for retention of topo I poisoning activity. The 6-bromo, 6-methoxy, or 6-phenyl derivatives of both 5-bromo- and 5-phenylterbenzimidazole were synthesized and evaluated for topo I poisoning activity, as well as their cytotoxicity toward human lymphoblastoma cells. The data indicate that such derivatives do retain similar topo I poisoning activity and possess cytotoxicity equivalent to either 5-bromo- or 5-phenylterbenzimidazole. Significant enhancement in the topoisomerase I poisoning activity and cytotoxicity of 5-phenylterbenzimidazole is observed when the 2″-position is substituted with either a chloro or trifluoromethyl substituent. The influence of such substituents on the biological activity of 5,6-dibromoterbenzimidazole (6a) was also explored. In the case of either 2″-chloro-5,6-dibromoterbenzimidazole (6b) or 2″-trifluoromethyl-5,6-dibromoterbenzimidazole (6c), topoisomerase I poisoning was not enhanced relative to6a. While cytotoxicity toward RPMI 8402 was also not significantly affected, comparative studies performed against several solid human tumor cell lines did reveal a significant increase in cytotoxicity observed for 6cas compared to 6a. Bioorganic & Medicinal Chemistry Letters 2000 E-Article NonPeerReviewed text en http://ir.unimas.my/id/eprint/2497/1/Topoisomerase%20I%20inhibition%20and%20cytotoxicity%20of%205-Bromo-%20and%205-Phenylterbenzimidazoles.pdf Rangarajan, M. and Kim, J.S. and Sim, S.P and Liu, A. and Liu, L.F. and LaVoie, E.J. (2000) Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles. Bioorganic & Medicinal Chemistry, 8 (11). pp. 2591-2600.
institution Universiti Malaysia Sarawak
building Centre for Academic Information Services (CAIS)
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Malaysia Sarawak
content_source UNIMAS Institutional Repository
url_provider http://ir.unimas.my/
language English
topic QD Chemistry
R Medicine (General)
spellingShingle QD Chemistry
R Medicine (General)
Rangarajan, M.
Kim, J.S.
Sim, S.P
Liu, A.
Liu, L.F.
LaVoie, E.J.
Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
description Topoisomerase I is an enzyme that is essential for maintaining the three-dimensional structure of DNA during the processes of transcription, translation and mitosis. With the introduction of new clinical agents that are effective in poisoning topoisomerase I, this enzyme has proved to be an attractive molecular target in the development of anticancer drugs. Several terbenzimidazoles have been identified as potent topoisomerase I poisons. Structure–activity data on various terbenzimidazoles have revealed that the presence of lipophilic substituents at the 5-position of various terbenzimidazoles correlates with enhanced cytotoxicity. While the effect of having substituents at both the 5- and 6-positions had not been evaluated, previous studies did indicate that the presence of a fused benzo-ring at the 5,6-position results in a significant decrease in topoisomerase I poisoning activity and cytotoxicity. In the present study we investigated whether substituents at both the 5- and 6-positions of varied terbenzimidazoles would allow for retention of topo I poisoning activity. The 6-bromo, 6-methoxy, or 6-phenyl derivatives of both 5-bromo- and 5-phenylterbenzimidazole were synthesized and evaluated for topo I poisoning activity, as well as their cytotoxicity toward human lymphoblastoma cells. The data indicate that such derivatives do retain similar topo I poisoning activity and possess cytotoxicity equivalent to either 5-bromo- or 5-phenylterbenzimidazole. Significant enhancement in the topoisomerase I poisoning activity and cytotoxicity of 5-phenylterbenzimidazole is observed when the 2″-position is substituted with either a chloro or trifluoromethyl substituent. The influence of such substituents on the biological activity of 5,6-dibromoterbenzimidazole (6a) was also explored. In the case of either 2″-chloro-5,6-dibromoterbenzimidazole (6b) or 2″-trifluoromethyl-5,6-dibromoterbenzimidazole (6c), topoisomerase I poisoning was not enhanced relative to6a. While cytotoxicity toward RPMI 8402 was also not significantly affected, comparative studies performed against several solid human tumor cell lines did reveal a significant increase in cytotoxicity observed for 6cas compared to 6a.
format E-Article
author Rangarajan, M.
Kim, J.S.
Sim, S.P
Liu, A.
Liu, L.F.
LaVoie, E.J.
author_facet Rangarajan, M.
Kim, J.S.
Sim, S.P
Liu, A.
Liu, L.F.
LaVoie, E.J.
author_sort Rangarajan, M.
title Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
title_short Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
title_full Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
title_fullStr Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
title_full_unstemmed Topoisomerase I inhibition and cytotoxicity of 5-Bromo- and 5-Phenylterbenzimidazoles
title_sort topoisomerase i inhibition and cytotoxicity of 5-bromo- and 5-phenylterbenzimidazoles
publisher Bioorganic & Medicinal Chemistry Letters
publishDate 2000
url http://ir.unimas.my/id/eprint/2497/1/Topoisomerase%20I%20inhibition%20and%20cytotoxicity%20of%205-Bromo-%20and%205-Phenylterbenzimidazoles.pdf
http://ir.unimas.my/id/eprint/2497/
_version_ 1644509104844046336