Novel organotin complexes with phenol and imidazole moieties for optimized antitumor properties
E A Nikitin
1
,
D B Shpakovsky
1
,
V Yu Tyurin
1
,
A A Kazak
1
,
Yu A Gracheva
1
,
V A Vasilichin
1
,
M S Pavlyukov
2
,
E.M. Mironova
1
,
V E Gontcharenko
1
,
K.A. Lyssenko
1
,
A A Antonets
1
,
L. G. Dubova
3
,
P N Shevtsov
3
,
E. F. Shevtsova
3
,
M A Shamraeva
4
,
A A Shtil
1, 5
,
E R Milaeva
1, 3
Publication type: Journal Article
Publication date: 2022-02-01
scimago Q3
wos Q2
SJR: 0.385
CiteScore: 4.1
Impact factor: 2.4
ISSN: 0022328X, 18728561
Materials Chemistry
Organic Chemistry
Biochemistry
Inorganic Chemistry
Physical and Theoretical Chemistry
Abstract
A series of novel imidazole-containing ligands and their organotin complexes were synthesized and characterized by NMR, IR, MALDI and elemental analysis. Redox behavior was studied by cyclic voltammetry (CV). Antioxidant properties were estimated in model reactions of single-electron reduction (CUPRAC-test), scavenging of 2,2-diphenyl-1-picrylhydrazyl (DPPH) and O2−. radical anion, enzymatic oxidation of linoleic acid by lipoxygenase and Fe3+-induced lipid peroxidation of rat liver homogenates. It was found that ligands and complexes both possess radical scavenging activity of prolonged action type. Compounds exhibited notable antioxidant activity in lipid peroxidation. Cytotoxicity was estimated in standard MTT-test on multiple cell lines. Compounds demonstrated high toxicity on colon carcinoma and breast cancer cells and based on obtained data, lead compound was proposed. Additional assays were carried out for the lead compound, including regular MTT-test on cancer cells possessing various resistant mechanisms and modified MTT-test on tumor tissue samples, obtained from patients as well as apoptosis and cell cycle studies. All organotin complexes were also studied for their influence on tubulin polymerization. It was demonstrated that obtained compounds demonstrate unorthodox activity, promoting microtubules assembly rate instead of inhibiting it. Significant influence of compound 5 on G2/M phase of cell cycle is in accordance with influence on tubulin polymerization and lets us to mark synthesized compounds as mitotic poisons. The results open up the scopes for the search of novel antitumor agents for treatment of advanced forms of cancer.
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15
Total citations:
15
Citations from 2025:
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(13.33%)
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GOST
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Nikitin E. A. et al. Novel organotin complexes with phenol and imidazole moieties for optimized antitumor properties // Journal of Organometallic Chemistry. 2022. Vol. 959. p. 122212.
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Nikitin E. A., Shpakovsky D. B., Tyurin V. Yu., Kazak A. A., Gracheva Yu. A., Vasilichin V. A., Pavlyukov M. S., Mironova E., Gontcharenko V. E., Lyssenko K., Antonets A. A., Dubova L. G., Shevtsov P. N., Shevtsova E. F., Shamraeva M. A., Shtil A. A., Milaeva E. R. Novel organotin complexes with phenol and imidazole moieties for optimized antitumor properties // Journal of Organometallic Chemistry. 2022. Vol. 959. p. 122212.
Cite this
RIS
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TY - JOUR
DO - 10.1016/j.jorganchem.2021.122212
UR - https://doi.org/10.1016/j.jorganchem.2021.122212
TI - Novel organotin complexes with phenol and imidazole moieties for optimized antitumor properties
T2 - Journal of Organometallic Chemistry
AU - Nikitin, E A
AU - Shpakovsky, D B
AU - Tyurin, V Yu
AU - Kazak, A A
AU - Gracheva, Yu A
AU - Vasilichin, V A
AU - Pavlyukov, M S
AU - Mironova, E.M.
AU - Gontcharenko, V E
AU - Lyssenko, K.A.
AU - Antonets, A A
AU - Dubova, L. G.
AU - Shevtsov, P N
AU - Shevtsova, E. F.
AU - Shamraeva, M A
AU - Shtil, A A
AU - Milaeva, E R
PY - 2022
DA - 2022/02/01
PB - Elsevier
SP - 122212
VL - 959
SN - 0022-328X
SN - 1872-8561
ER -
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BibTex (up to 50 authors)
Copy
@article{2022_Nikitin,
author = {E A Nikitin and D B Shpakovsky and V Yu Tyurin and A A Kazak and Yu A Gracheva and V A Vasilichin and M S Pavlyukov and E.M. Mironova and V E Gontcharenko and K.A. Lyssenko and A A Antonets and L. G. Dubova and P N Shevtsov and E. F. Shevtsova and M A Shamraeva and A A Shtil and E R Milaeva},
title = {Novel organotin complexes with phenol and imidazole moieties for optimized antitumor properties},
journal = {Journal of Organometallic Chemistry},
year = {2022},
volume = {959},
publisher = {Elsevier},
month = {feb},
url = {https://doi.org/10.1016/j.jorganchem.2021.122212},
pages = {122212},
doi = {10.1016/j.jorganchem.2021.122212}
}
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