том 49 издание 42 страницы 14891-14907

Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation

Тип публикацииJournal Article
Дата публикации2020-09-29
SCImago Q2
WOS Q1
БС1
SJR0.581
CiteScore6
Impact factor3.3
ISSN14779226, 14779234
Inorganic Chemistry
Краткое описание
A rational approach was adopted to design high-potential metal-based antitumor agents. A series of organometallic Pd(II) complexes with a general formula of [Pd{κ2(C,C)-[(C6H4-2)PPh2]CH(CO)C6H4Ph-4}{κ2(N,O)}] (N,O = alanine (Pd-A), valine (Pd-V), leucine (Pd-L), L-isoleucine (Pd-I) and phenylalanine (Pd-F)) were prepared by cyclopalladation of the phosphorus ylide, bridge cleavage reaction and subsequent chelation of natural α-amino acids. The complexes were fully identified using IR and multinuclear 1H, 13C, 31P NMR spectroscopic methods. X-ray crystallography exhibited that the Pd(II) atom is located in a slightly distorted square-planar environment surrounded by C,C-orthometallated phosphorus ylide as well as NO-pendant amino acid functionality. In vitro cytotoxicity evaluation of new cyclometallated Pd(II) complexes toward a human leukemia (K562) cancer cell line indicated promising results. The highest cytotoxic activity was discovered in the case of phenylalanine (CH2C6H5). IC50 values of this complex on a panel of human tumor cell lines representative of liver (HepG2), breast (SKBR-3), and ovarian (A2780-Resistance/Sensitive) cancers also indicated promising antitumor effects in comparison with standard cisplatin. The binding interaction ability of the phenylalanine-containing orthopalladated complex, as the most efficient compound, with calf-thymus deoxyribonucleic acid (CT-DNA) and bovine serum albumin (BSA) was investigated. UV-Vis spectroscopy, competitive emission titration, and circular dichroism (CD) techniques demonstrated the intercalative binding of the Pd(II) complex with DNA. Molecular docking studies also fully agreed with the experimental data. Examination of the reactivity towards the protein BSA revealed that the static quenching mechanism of BSA intrinsic fluorescence by the Pd(II) complex with a binding constant (Kb) of ∼105 is indicative of the high affinity of the complex. The competitive binding experiment using site markers with definite binding sites demonstrated that the hydrophobic cavities of site I (subdomain IIA) are responsible for the bimolecular interaction between protein BSA and the complex. Molecular docking studies effectively confirmed the significance of hydrophobic interactions in Pd(II)–BSA binding. The results of this study could greatly contribute to exploring new potent metal-based anticancer drugs.
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Abedanzadeh S. et al. Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation // Dalton Transactions. 2020. Vol. 49. No. 42. pp. 14891-14907.
ГОСТ со всеми авторами (до 50) Скопировать
Abedanzadeh S. et al. Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation // Dalton Transactions. 2020. Vol. 49. No. 42. pp. 14891-14907.
RIS |
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TY - JOUR
DO - 10.1039/d0dt02304c
UR - https://xlink.rsc.org/?DOI=D0DT02304C
TI - Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation
T2 - Dalton Transactions
AU - Abedanzadeh, Sedigheh
AU - Karami, Kazem
AU - Rahimi, Mostafa
AU - Edalati, Masoud
AU - Abedanzadeh, Mozhgan
AU - Tamaddon, Ali‐Mohammad
AU - Jahromi, Maryam Dehdashti
AU - Amirghofran, Zahra
AU - Lipkowski, Janusz
AU - Lyczko, Krzysztof
PY - 2020
DA - 2020/09/29
PB - Royal Society of Chemistry (RSC)
SP - 14891-14907
IS - 42
VL - 49
PMID - 33075117
SN - 1477-9226
SN - 1477-9234
ER -
BibTex |
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@article{2020_Abedanzadeh,
author = {Sedigheh Abedanzadeh and Kazem Karami and Mostafa Rahimi and Masoud Edalati and Mozhgan Abedanzadeh and Ali‐Mohammad Tamaddon and Maryam Dehdashti Jahromi and Zahra Amirghofran and Janusz Lipkowski and Krzysztof Lyczko and others},
title = {Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation},
journal = {Dalton Transactions},
year = {2020},
volume = {49},
publisher = {Royal Society of Chemistry (RSC)},
month = {sep},
url = {https://xlink.rsc.org/?DOI=D0DT02304C},
number = {42},
pages = {14891--14907},
doi = {10.1039/d0dt02304c}
}
MLA
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Abedanzadeh, Sedigheh, et al. “Potent cyclometallated Pd(ii) antitumor complexes bearing α-amino acids: synthesis, structural characterization, DNA/BSA binding, cytotoxicity and molecular dynamics simulation.” Dalton Transactions, vol. 49, no. 42, Sep. 2020, pp. 14891-14907. https://xlink.rsc.org/?DOI=D0DT02304C.
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