1-Hydroxyanthraquinones Containing Aryl Substituents as Potent and Selective Anticancer Agents

Nafisa S Sirazhetdinova; Victor A Savelyev; Tatyana S Frolova; Dmitry S Baev; Lyubov S Klimenko; Ivan V Chernikov; Olga S Oleshko; Teresa A Sarojan; Andrey G Pokrovskii; Elvira E Shults

doi:10.3390/molecules25112547

1-Hydroxyanthraquinones Containing Aryl Substituents as Potent and Selective Anticancer Agents

Molecules. 2020 May 29;25(11):2547. doi: 10.3390/molecules25112547.

Affiliations

¹ Laboratory of Medicinal Chemistry, N.N. Vorozhtsov Novosibirsk Institute of Organic Chemistry, Siberian Branch of the Russian Academy of Sciences, Lavrentyev Ave, 9, 630090 Novosibirsk, Russia.
² The Federal Research Center Institute of Cytology and Genetics, Acad. Lavrentyev Ave., 10, 630090, Novosibirsk, Russia.
³ Novosibirsk State University, Pirogova Str. 1, 630090 Novosibirsk, Russia.
⁴ Yugra State University, 628012, Khanty-Mansiysk, Russia.
⁵ Institute of Chemical Biology and Fundamental Medicine Siberian Branch of the Russian Academy of Sciences, Lavrentyev Ave, 9, 630090 Novosibirsk, Russia.

Abstract

A series of 1,2-, 1,4-disubstituted or 1,2,4-trisubstituted anthraquinone-based compounds was designed, synthesized, characterized and biologically evaluated for anticancer efficacy. 2- or 4-arylated 1-hydroxy-9,10-antraquinones (anthracene-9,10-diones) were prepared by Suzuki-Miyaura cross-coupling reaction of 1-hydroxy-2-bromoanthraquinone, 1-hydroxy-4-iodoanthraquinone or 1-hydroxy-2,4-dibromoanthraquinone with arylboronic acids. The cross-coupling reaction of 2,4-dibromo-9,10-anthraquinone with arylboronic acids provide a convenient approach to 2,4-bis arylated 1-hydroxyanthraquinones with a variety of aryl substituent in the 2 and 4 position. The cytotoxicity of new anthraquinone derivatives was evaluated using the conventional MTT assays. The data revealed that six of the aryl substituted compounds among the entire series 3, 15, 16, 25, 27, 28 were comparable potent with the commercially available reference drug doxorubicin on the human glioblastoma cells SNB-19, prostate cancer DU-145 or breast cancer cells MDA-MB-231 and were relatively safe towards human telomerase (h-TERT)immortalized lung fibroblasts cells. The results suggested that the in vitro antitumor activity of synthesized 2-aryl, 4-aryl- and 2,4-diaryl substituted 1-hydroxyanthraquinones depends on the nature of the substituent within the cyclic backbone. Docking interaction of 2-, 4-substituted and 2,4-disubstituted 1-hydroxyanthraquinones indicates intercalative mode of binding of compounds with DNA topoisomerase. The interaction with the DNA of 4-aryl-13, 15, 16 and 4-(furan-3-yl)-23 1-hydroxyanthraquinones was experimentally confirmed through a change in electroforetic mobility. Further experiments with 1-hydroxy-4-phenyl-anthraquinone 13 demonstrated that the compound induced cell cycle arrest at sub-G1 phase in DU-145 cells in the concentration 1.1 μM, which is probably achieved by inducing apoptosis. 4-Arylsubstituted 1-hydroxyanthraquinones 13 and 16 induced the enhancement of DNA synthesis on SNB19 cell lines.

Keywords: DNA binding; Suzuki cross-coupling reaction; anthraquinones; cytotoxicity.

MeSH terms

Anthraquinones / chemical synthesis*
Anthraquinones / chemistry
Antineoplastic Agents / pharmacology*
Apoptosis
Cell Line, Tumor
Cell Proliferation / drug effects
DNA / chemistry
Drug Design
Drug Screening Assays, Antitumor
Humans
Magnetic Resonance Spectroscopy
Molecular Docking Simulation
Molecular Structure
Structure-Activity Relationship
Telomerase / metabolism

Substances

Anthraquinones
Antineoplastic Agents
DNA
Telomerase
1-hydroxyanthraquinone

Grants and funding

18-13-00361/Russian Science Foundation