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Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA
Dimorfolido-N-trichloroacetylphosphorylamide (HL1) and dimorfolido-N-benzoylphosphorylamide (HL2) as representatives of carbacylamidophosphates were synthesized and identified by the methods of IR, (1)H, and (31)P NMR spectroscopy. In vitro HL1 and HL2 at 1 mM concentration caused cell specific and...
Autores principales: | , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
Springer US
2017
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5315654/ https://www.ncbi.nlm.nih.gov/pubmed/28235359 http://dx.doi.org/10.1186/s11671-017-1893-3 |
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author | Prylutska, S. Grynyuk, I. Grebinyk, A. Hurmach, V. Shatrava, Iu. Sliva, T. Amirkhanov, V. Prylutskyy, Yu. Matyshevska, O. Slobodyanik, M. Frohme, M. Ritter, U. |
author_facet | Prylutska, S. Grynyuk, I. Grebinyk, A. Hurmach, V. Shatrava, Iu. Sliva, T. Amirkhanov, V. Prylutskyy, Yu. Matyshevska, O. Slobodyanik, M. Frohme, M. Ritter, U. |
author_sort | Prylutska, S. |
collection | PubMed |
description | Dimorfolido-N-trichloroacetylphosphorylamide (HL1) and dimorfolido-N-benzoylphosphorylamide (HL2) as representatives of carbacylamidophosphates were synthesized and identified by the methods of IR, (1)H, and (31)P NMR spectroscopy. In vitro HL1 and HL2 at 1 mM concentration caused cell specific and time-dependent decrease of leukemic cell viability. Compounds caused the similar gradual decrease of Jurkat cells viability at 72 h (by 35%). HL1 had earlier and more profound toxic effect as compared to HL2 regardless on leukemic cell line. Viability of Molt-16 and CCRF-CEM cells under the action of HL1 was decreased at 24 h (by 32 and 45%, respectively) with no substantial further reducing up to 72 h. Toxic effect of HL2 was detected only at 72 h of incubation of Jurkat and Molt-16 cells (cell viability was decreased by 40 and 45%, respectively). It was shown that C(60) fullerene enhanced the toxic effect of HL2 on leukemic cells. Viability of Jurkat and CCRF-CEM cells at combined action of C(60) fullerene and HL2 was decreased at 72 h (by 20 and 24%, respectively) in comparison with the effect of HL2 taken separately. In silico study showed that HL1 and HL2 can interact with DNA and form complexes with DNA both separately and in combination with C(60) fullerene. More stable complexes are formed when DNA interacts with HL1 or C(60) + HL2 structure. Strong stacking interactions can be formed between HL2 and C(60) fullerene. Differences in the types of identified bonds and ways of binding can determine distinction in cytotoxic effects of studied compounds. |
format | Online Article Text |
id | pubmed-5315654 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2017 |
publisher | Springer US |
record_format | MEDLINE/PubMed |
spelling | pubmed-53156542017-03-02 Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA Prylutska, S. Grynyuk, I. Grebinyk, A. Hurmach, V. Shatrava, Iu. Sliva, T. Amirkhanov, V. Prylutskyy, Yu. Matyshevska, O. Slobodyanik, M. Frohme, M. Ritter, U. Nanoscale Res Lett Nano Express Dimorfolido-N-trichloroacetylphosphorylamide (HL1) and dimorfolido-N-benzoylphosphorylamide (HL2) as representatives of carbacylamidophosphates were synthesized and identified by the methods of IR, (1)H, and (31)P NMR spectroscopy. In vitro HL1 and HL2 at 1 mM concentration caused cell specific and time-dependent decrease of leukemic cell viability. Compounds caused the similar gradual decrease of Jurkat cells viability at 72 h (by 35%). HL1 had earlier and more profound toxic effect as compared to HL2 regardless on leukemic cell line. Viability of Molt-16 and CCRF-CEM cells under the action of HL1 was decreased at 24 h (by 32 and 45%, respectively) with no substantial further reducing up to 72 h. Toxic effect of HL2 was detected only at 72 h of incubation of Jurkat and Molt-16 cells (cell viability was decreased by 40 and 45%, respectively). It was shown that C(60) fullerene enhanced the toxic effect of HL2 on leukemic cells. Viability of Jurkat and CCRF-CEM cells at combined action of C(60) fullerene and HL2 was decreased at 72 h (by 20 and 24%, respectively) in comparison with the effect of HL2 taken separately. In silico study showed that HL1 and HL2 can interact with DNA and form complexes with DNA both separately and in combination with C(60) fullerene. More stable complexes are formed when DNA interacts with HL1 or C(60) + HL2 structure. Strong stacking interactions can be formed between HL2 and C(60) fullerene. Differences in the types of identified bonds and ways of binding can determine distinction in cytotoxic effects of studied compounds. Springer US 2017-02-17 /pmc/articles/PMC5315654/ /pubmed/28235359 http://dx.doi.org/10.1186/s11671-017-1893-3 Text en © The Author(s). 2017 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. |
spellingShingle | Nano Express Prylutska, S. Grynyuk, I. Grebinyk, A. Hurmach, V. Shatrava, Iu. Sliva, T. Amirkhanov, V. Prylutskyy, Yu. Matyshevska, O. Slobodyanik, M. Frohme, M. Ritter, U. Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title | Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title_full | Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title_fullStr | Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title_full_unstemmed | Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title_short | Cytotoxic Effects of Dimorfolido-N-Trichloroacetylphosphorylamide and Dimorfolido-N-Benzoylphosphorylamide in Combination with C(60) Fullerene on Leukemic Cells and Docking Study of Their Interaction with DNA |
title_sort | cytotoxic effects of dimorfolido-n-trichloroacetylphosphorylamide and dimorfolido-n-benzoylphosphorylamide in combination with c(60) fullerene on leukemic cells and docking study of their interaction with dna |
topic | Nano Express |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5315654/ https://www.ncbi.nlm.nih.gov/pubmed/28235359 http://dx.doi.org/10.1186/s11671-017-1893-3 |
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