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том 50 издание 20 страницы 10284-10291

New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study

Тип публикацииJournal Article
Дата публикации2011-09-16
scimago Q1
wos Q1
БС1
SJR0.928
CiteScore7.6
Impact factor4.7
ISSN00201669, 1520510X
Inorganic Chemistry
Physical and Theoretical Chemistry
Краткое описание
Following the discovery of cisplatin, much effort has been devoted to the exploration of transition metal complexes as cytotoxic agents. We have recently introduced the highly efficient C(2)-symmetrical salan-Ti(IV) family of complexes, demonstrating high cytotoxicity toward colon and ovarian cells and enhanced hydrolytic stability in mixed organic/water solutions. The effect of stereochemistry is hereby reported, by comparing the cytotoxic activity and hydrolysis of pure enantiomers and their racemic mixture for four complexes of this family with different aromatic substitutions: para-Me, para-Cl, ortho-Cl, and ortho-OMe. These complexes include the trans-diaminocyclohexyl bridge, which enables ligand-to-metal chiral induction to give solely the Δ isomer when starting from the R,R ligand and vice versa. Different activity is obtained for the different stereochemical forms (Δ, Λ, and rac) in two of the four complexes, where for the other two either all forms are inactive or all are highly active. Additionally, where not all are of similar activity, the racemic mixture is the least active of the three. We therefore conclude that the salan ligand is essential for the fruitful biological interaction, which probably involves a chiral cellular target. The activity of the racemate differing from that expected from a simple mixture of enantiomers operating separately may be explained by the involvement of a polynuclear active species, where different metal centers might be of different configurations. This is particularly supported by the different polynuclear products of hydrolysis obtained from an optically pure complex and from the racemic one, as analyzed crystallographically. The former is an all-R,R chiral C(1)-symmetrical homodimer, while the latter is an achiral R,R-S,SC(i)-symmetrical heterodimer obtained through chiral recognition.
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Manna C. M., Armony G., Tshuva E. New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study // Inorganic Chemistry. 2011. Vol. 50. No. 20. pp. 10284-10291.
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Manna C. M., Armony G., Tshuva E. New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study // Inorganic Chemistry. 2011. Vol. 50. No. 20. pp. 10284-10291.
RIS |
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TY - JOUR
DO - 10.1021/ic201340m
UR - https://doi.org/10.1021/ic201340m
TI - New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study
T2 - Inorganic Chemistry
AU - Manna, Cesar M
AU - Armony, Gad
AU - Tshuva, Edit
PY - 2011
DA - 2011/09/16
PB - American Chemical Society (ACS)
SP - 10284-10291
IS - 20
VL - 50
PMID - 21923127
SN - 0020-1669
SN - 1520-510X
ER -
BibTex |
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BibTex (до 50 авторов) Скопировать
@article{2011_Manna,
author = {Cesar M Manna and Gad Armony and Edit Tshuva},
title = {New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study},
journal = {Inorganic Chemistry},
year = {2011},
volume = {50},
publisher = {American Chemical Society (ACS)},
month = {sep},
url = {https://doi.org/10.1021/ic201340m},
number = {20},
pages = {10284--10291},
doi = {10.1021/ic201340m}
}
MLA
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Manna, Cesar M., et al. “New Insights on the Active Species and Mechanism of Cytotoxicity of Salan-Ti(IV) Complexes: A Stereochemical Study.” Inorganic Chemistry, vol. 50, no. 20, Sep. 2011, pp. 10284-10291. https://doi.org/10.1021/ic201340m.