Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand

Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand

A series of ternary copper(II)-1,10-phenanthroline complexes with glycine and methylated glycine derivatives, [Cu(phen)(aa)(H2O)]NO3·xH2O 1–4 (amino acid (aa): glycine (gly), 1; dl-alanine (dl-ala), 2; 2,2-dimethylglycine (C-dmg), 3; sarcosine (sar), 4), were synthesized and characterized by FTIR, e...

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Main Authors: Seng, Hoi-Ling, Wang, Wai-San, Kong, Siew-Ming, Alan Ong, Han-Kiat, Win, Yip-Foo, Raja Abd. Rahman, Raja Noor Zaliha, Chikira, Makoto, Leong, Weng Kee, Ahmad, Munirah, Khoo, Alan Soo-Beng, Ng, Chew-Hee
Other Authors: School of Physical and Mathematical Sciences
Format: Article
Language:English
Published: 2013
Online Access:https://hdl.handle.net/10356/98845
http://hdl.handle.net/10220/12861
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-988452020-03-07T12:34:43Z Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand Seng, Hoi-Ling Wang, Wai-San Kong, Siew-Ming Alan Ong, Han-Kiat Win, Yip-Foo Raja Abd. Rahman, Raja Noor Zaliha Chikira, Makoto Leong, Weng Kee Ahmad, Munirah Khoo, Alan Soo-Beng Ng, Chew-Hee School of Physical and Mathematical Sciences A series of ternary copper(II)-1,10-phenanthroline complexes with glycine and methylated glycine derivatives, [Cu(phen)(aa)(H2O)]NO3·xH2O 1–4 (amino acid (aa): glycine (gly), 1; dl-alanine (dl-ala), 2; 2,2-dimethylglycine (C-dmg), 3; sarcosine (sar), 4), were synthesized and characterized by FTIR, elemental analysis, electrospray ionization–mass spectra (ESI–MS), UV–visible spectroscopy and molar conductivity measurement. The determined X-ray crystallographic structures of 2 and 3 show each to consist of distorted square pyramidal [Cu(phen)(aa)(H2O)]+ cation, a nitrate counter anion, and with or without lattice water, similar to previously reported structure of [Cu(phen)(gly)(H2O)]NO3·1½H2O. It is found that 1–4 exist as 1:1 electrolytes in aqueous solution, and the cationic copper(II) complexes are at least stable up to 24 h. Positive-ion ESI–MS spectra show existence of only undissociated [Cu(phen)(aa)]+ species. Electron paramagnetic resonance, gel electrophoresis, fluorescence quenching, and restriction enzyme inhibition assay were used to study the binding interaction, binding affinity and selectivity of these complexes for various types of B-form DNA duplexes and G-quadruplex. All complexes can bind selectively to DNA by intercalation and electrostatic forces, and inhibit topoisomerase I. The effect of the methyl substituents of the coordinated amino acid in the above complexes on these biological properties are presented and discussed. The IC50 values (24 h) of 1–4 for nasopharyngeal cancer cell line HK1 are in the range 2.2–5.2 μM while the corresponding values for normal cell line NP69 are greater than 13.0 μM. All complexes, at 5 μM, induced 41–60 % apoptotic cell death in HK1 cells but no significant cell death in NP69 cells. 2013-08-02T03:45:13Z 2019-12-06T20:00:15Z 2013-08-02T03:45:13Z 2019-12-06T20:00:15Z 2012 2012 Journal Article Seng, H. L., Wang, W. S., Kong, S. M., Alan Ong, H. K., Win, Y. F., Raja Abd. Rahman, R. N. Z., Chikira, M., Leong, W. K., Ahmad, M., Khoo, A. S. B.,& Ng, C. H. (2012). Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand. BioMetals, 25(5), 1061-1081. https://hdl.handle.net/10356/98845 http://hdl.handle.net/10220/12861 10.1007/s10534-012-9572-4 en BioMetals
institution Nanyang Technological University
building NTU Library
country Singapore
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description A series of ternary copper(II)-1,10-phenanthroline complexes with glycine and methylated glycine derivatives, [Cu(phen)(aa)(H2O)]NO3·xH2O 1–4 (amino acid (aa): glycine (gly), 1; dl-alanine (dl-ala), 2; 2,2-dimethylglycine (C-dmg), 3; sarcosine (sar), 4), were synthesized and characterized by FTIR, elemental analysis, electrospray ionization–mass spectra (ESI–MS), UV–visible spectroscopy and molar conductivity measurement. The determined X-ray crystallographic structures of 2 and 3 show each to consist of distorted square pyramidal [Cu(phen)(aa)(H2O)]+ cation, a nitrate counter anion, and with or without lattice water, similar to previously reported structure of [Cu(phen)(gly)(H2O)]NO3·1½H2O. It is found that 1–4 exist as 1:1 electrolytes in aqueous solution, and the cationic copper(II) complexes are at least stable up to 24 h. Positive-ion ESI–MS spectra show existence of only undissociated [Cu(phen)(aa)]+ species. Electron paramagnetic resonance, gel electrophoresis, fluorescence quenching, and restriction enzyme inhibition assay were used to study the binding interaction, binding affinity and selectivity of these complexes for various types of B-form DNA duplexes and G-quadruplex. All complexes can bind selectively to DNA by intercalation and electrostatic forces, and inhibit topoisomerase I. The effect of the methyl substituents of the coordinated amino acid in the above complexes on these biological properties are presented and discussed. The IC50 values (24 h) of 1–4 for nasopharyngeal cancer cell line HK1 are in the range 2.2–5.2 μM while the corresponding values for normal cell line NP69 are greater than 13.0 μM. All complexes, at 5 μM, induced 41–60 % apoptotic cell death in HK1 cells but no significant cell death in NP69 cells.
author2 School of Physical and Mathematical Sciences
author_facet School of Physical and Mathematical Sciences
Seng, Hoi-Ling
Wang, Wai-San
Kong, Siew-Ming
Alan Ong, Han-Kiat
Win, Yip-Foo
Raja Abd. Rahman, Raja Noor Zaliha
Chikira, Makoto
Leong, Weng Kee
Ahmad, Munirah
Khoo, Alan Soo-Beng
Ng, Chew-Hee
format Article
author Seng, Hoi-Ling
Wang, Wai-San
Kong, Siew-Ming
Alan Ong, Han-Kiat
Win, Yip-Foo
Raja Abd. Rahman, Raja Noor Zaliha
Chikira, Makoto
Leong, Weng Kee
Ahmad, Munirah
Khoo, Alan Soo-Beng
Ng, Chew-Hee
spellingShingle Seng, Hoi-Ling
Wang, Wai-San
Kong, Siew-Ming
Alan Ong, Han-Kiat
Win, Yip-Foo
Raja Abd. Rahman, Raja Noor Zaliha
Chikira, Makoto
Leong, Weng Kee
Ahmad, Munirah
Khoo, Alan Soo-Beng
Ng, Chew-Hee
Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
author_sort Seng, Hoi-Ling
title Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
title_short Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
title_full Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
title_fullStr Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
title_full_unstemmed Biological and cytoselective anticancer properties of copper(II)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
title_sort biological and cytoselective anticancer properties of copper(ii)-polypyridyl complexes modulated by auxiliary methylated glycine ligand
publishDate 2013
url https://hdl.handle.net/10356/98845
http://hdl.handle.net/10220/12861
_version_ 1681041796712366080

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