Design, synthesis, and molecular docking study of new tyrosyl-DNA phosphodiesterase 1 (TDP1) inhibitors combining resin acids and adamantane moietiesстатья
Статья опубликована в высокорейтинговом журнале
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Статья опубликована в журнале из списка Web of Science и/или Scopus
Дата последнего поиска статьи во внешних источниках: 30 июня 2021 г.
Авторы:
Kovaleva K.,
Yarovaya O.,
Ponomarev K.,
Cheresiz S.,
Azimirad A.,
Chernyshova I.,
Zakharenko A.,
Konev V.,
Khlebnikova T.,
Mozhaytsev E.,
Suslov E.,
Nilov D.,
Švedas V.,
Pokrovsky A.,
Lavrik O.,
Salakhutdinov N.
Аннотация:In this paper, a series of novel abietyl and dehydroabietyl ureas, thioureas, amides, and thioamides bearing adamantane moieties were designed, synthesized, and evaluated for their inhibitory activities against tyrosil-DNA-phosphodiesterase 1 (TDP1). The synthesized compounds were able to inhibit TDP1 at micromolar concentrations (0.19–2.3 µM) and demonstrated low cytotoxicity in the T98G glioma cell line. The effect of the terpene fragment, the linker structure, and the adamantane residue on the biological properties of the new compounds was investigated. Based on molecular docking results, we suppose that adamantane derivatives of resin acids bind to the TDP1 covalent intermediate, forming a hydrogen bond with Ser463 and hydrophobic contacts with the Phe259 and Trp590 residues and the oligonucleotide fragment of the substrate.