Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA
A series of substituted salicylaldehyde dibenzyl semicarbazones [RC6H3(OH)CH[double bond, length as m-dash]N–NHCON(CH2Ph)2] and their copper(II) complexes were synthesized and characterized. The chloridocopper(II) complexes of the 4-OH and 5-OH substituted ligands (complexes 9 and 7) show modest aff...
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sg-ntu-dr.10356-1044602023-12-29T06:47:34Z Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA Klejevskaja, Beata Munira Haidad Ali, Siti Yan, Yaw-Kai Lee, Peter P. F. Khong, Kenny Zhi Xiang Alam Sk, Mahasin Lim, Kok Hwa Vilar, Ramon School of Chemical and Biomedical Engineering National Institute of Education DRNTU::Engineering::Bioengineering A series of substituted salicylaldehyde dibenzyl semicarbazones [RC6H3(OH)CH[double bond, length as m-dash]N–NHCON(CH2Ph)2] and their copper(II) complexes were synthesized and characterized. The chloridocopper(II) complexes of the 4-OH and 5-OH substituted ligands (complexes 9 and 7) show modest affinity and good selectivity (over duplex DNA) for the quadruplex formed from the 22AG human telomeric (HTelo) DNA sequence. Substitution of the chlorido ligands of these two complexes with pyridine yielded derivatives (7-py and 9-py) with increased affinity for HTelo. These derivatives also show good selectivity for HTelo over calf-thymus DNA (170- and 211-fold, respectively). The X-ray crystal structures of 9 and 9-py were determined. Molecular docking studies based on these structures show that the complexes stack on the 5′-end of the HTelo quadruplex, with the hydroxyl group forming a hydrogen bond with a guanine residue. Complexes 7, 9, 7-py and 9-py display significant cytotoxicity against MOLT-4 human leukaemia cells. Interestingly, they have low to negligible cytotoxicity against the non-cancerous IMR-90 human fibroblasts. NMRC (Natl Medical Research Council, S’pore) Accepted version 2014-07-14T08:36:41Z 2019-12-06T21:33:15Z 2014-07-14T08:36:41Z 2019-12-06T21:33:15Z 2014 2014 Commentary Journal Article Munira Haidad Ali, S., Yan, Y. K., Lee, P. P. F., Khong, K. Z. X., Alam Sk, M., Lim, K. H., Klejevskaja, B., & Vilar, R. (2014). Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones: synthesis, cytotoxicity and interaction with quadruplex DNA. Dalton Transactions, 43(3), 1449-1459. 1477-9226 https://hdl.handle.net/10356/104460 http://hdl.handle.net/10220/20209 10.1039/c3dt52297k en Dalton Transactions © 2014 Royal Society of Chemistry. This is the author created version of a work that has been peer reviewed and accepted for publication by Dalton Transactions, Royal Society of Chemistry. It incorporates referee’s comments but changes resulting from the publishing process, such as copyediting, structural formatting, may not be reflected in this document. The published version is available at: [http://dx.doi.org/10.1039/c3dt52297k]. application/pdf |
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DRNTU::Engineering::Bioengineering Klejevskaja, Beata Munira Haidad Ali, Siti Yan, Yaw-Kai Lee, Peter P. F. Khong, Kenny Zhi Xiang Alam Sk, Mahasin Lim, Kok Hwa Vilar, Ramon Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
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A series of substituted salicylaldehyde dibenzyl semicarbazones [RC6H3(OH)CH[double bond, length as m-dash]N–NHCON(CH2Ph)2] and their copper(II) complexes were synthesized and characterized. The chloridocopper(II) complexes of the 4-OH and 5-OH substituted ligands (complexes 9 and 7) show modest affinity and good selectivity (over duplex DNA) for the quadruplex formed from the 22AG human telomeric (HTelo) DNA sequence. Substitution of the chlorido ligands of these two complexes with pyridine yielded derivatives (7-py and 9-py) with increased affinity for HTelo. These derivatives also show good selectivity for HTelo over calf-thymus DNA (170- and 211-fold, respectively). The X-ray crystal structures of 9 and 9-py were determined. Molecular docking studies based on these structures show that the complexes stack on the 5′-end of the HTelo quadruplex, with the hydroxyl group forming a hydrogen bond with a guanine residue. Complexes 7, 9, 7-py and 9-py display significant cytotoxicity against MOLT-4 human leukaemia cells. Interestingly, they have low to negligible cytotoxicity against the non-cancerous IMR-90 human fibroblasts. |
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School of Chemical and Biomedical Engineering |
author_facet |
School of Chemical and Biomedical Engineering Klejevskaja, Beata Munira Haidad Ali, Siti Yan, Yaw-Kai Lee, Peter P. F. Khong, Kenny Zhi Xiang Alam Sk, Mahasin Lim, Kok Hwa Vilar, Ramon |
format |
Commentary Article |
author |
Klejevskaja, Beata Munira Haidad Ali, Siti Yan, Yaw-Kai Lee, Peter P. F. Khong, Kenny Zhi Xiang Alam Sk, Mahasin Lim, Kok Hwa Vilar, Ramon |
author_sort |
Klejevskaja, Beata |
title |
Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
title_short |
Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
title_full |
Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
title_fullStr |
Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
title_full_unstemmed |
Copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex DNA |
title_sort |
copper(ii) complexes of substituted salicylaldehyde dibenzyl semicarbazones : synthesis, cytotoxicity and interaction with quadruplex dna |
publishDate |
2014 |
url |
https://hdl.handle.net/10356/104460 http://hdl.handle.net/10220/20209 |
_version_ |
1787136520997568512 |