Adamantane-substituted purines and their β-cyclodextrin complexes: Synthesis and biological activity

Rouchal, Michal; Rudolfová, Jana; Kryštof, Vladimír; Vojáčková, Veronika; Čmelík, Richard; Vícha, Robert

dc.title	Adamantane-substituted purines and their β-cyclodextrin complexes: Synthesis and biological activity	en
dc.contributor.author	Rouchal, Michal
dc.contributor.author	Rudolfová, Jana
dc.contributor.author	Kryštof, Vladimír
dc.contributor.author	Vojáčková, Veronika
dc.contributor.author	Čmelík, Richard
dc.contributor.author	Vícha, Robert
dc.relation.ispartof	International Journal of Molecular Sciences
dc.identifier.issn	1661-6596 Scopus Sources, Sherpa/RoMEO, JCR
dc.identifier.issn	1422-0067 Scopus Sources, Sherpa/RoMEO, JCR
dc.date.issued	2021
utb.relation.volume	22
utb.relation.issue	23
dc.type	article
dc.language.iso	en
dc.publisher	MDPI
dc.identifier.doi	10.3390/ijms222312675
dc.relation.uri	https://www.mdpi.com/1422-0067/22/23/12675
dc.subject	adamantane	en
dc.subject	2,6,9-trisubstituted purine	en
dc.subject	cyclin-dependent kinase	en
dc.subject	cytotoxicity	en
dc.subject	β-cyclodextrin	en
dc.subject	molecular docking	en
dc.description.abstract	Cyclin-dependent kinases (CDKs) play an important role in the cell-division cycle. Synthetic inhibitors of CDKs are based on 2,6,9-trisubstituted purines and are developed as potential anticancer drugs; however, they have low solubility in water. In this study, we proved that the pharmaco-chemical properties of purine-based inhibitors can be improved by appropriate substitution with the adamantane moiety. We prepared ten new purine derivatives with adamantane skeletons that were linked at position 6 using phenylene spacers of variable geometry and polarity. We demonstrated that the adamantane skeleton does not compromise the biological activity, and some of the new purines displayed even higher inhibition activity towards CDK2/cyclin E than the parental compounds. These findings were supported by a docking study, which showed an adamantane scaffold inside the binding pocket participating in the complex stabilisation with non-polar interactions. In addition, we demonstrated that β-cyclodextrin (CD) increases the drug’s solubility in water, although this is at the cost of reducing the biochemical and cellular effect. Most likely, the drug concentration, which is necessary for target engagement, was decreased by competitive drug binding within the complex with β-CD. : © 2021 by the authors. Licensee MDPI, Basel, Switzerland.	en
utb.faculty	Faculty of Technology
dc.identifier.uri	http://hdl.handle.net/10563/1010661
utb.identifier.obdid	43883035
utb.identifier.scopus	2-s2.0-85119661216
utb.identifier.wok	000735654100001
utb.identifier.pubmed	34884480
utb.source	j-scopus
dc.date.accessioned	2021-12-02T12:03:14Z
dc.date.available	2021-12-02T12:03:14Z
dc.description.sponsorship	RVO: 68081715; Grantová Agentura České Republiky, GA ČR: GA 19-08410S; Univerzita Tomáše Bati ve Zlíně: IGA/FT/2021/001
dc.description.sponsorship	Internal Funding Agency of the Tomas Bata University in Zlin [IGA/FT/2021/001]; Czech Science FoundationGrant Agency of the Czech Republic [GA 19-08410S]; Institute of Analytical Chemistry of the Czech Academy of SciencesCzech Academy of Sciences [RVO: 68081715]
dc.rights	Attribution 4.0 International
dc.rights.uri	https://creativecommons.org/licenses/by/4.0/
dc.rights.access	openAccess
utb.ou	Department of Chemistry
utb.contributor.internalauthor	Rouchal, Michal
utb.contributor.internalauthor	Rudolfová, Jana
utb.contributor.internalauthor	Vícha, Robert
utb.fulltext.affiliation	Michal Rouchal 1 , Jana Rudolfová 1, Vladimír Kryštof 2, Veronika Vojáčková2, Richard Čmelík3 and Robert Vícha 1,* 1 Department of Chemistry, Faculty of Technology, Tomas Bata University in Zlín, Vavrečkova 275, 760 01 Zlín, Czech Republic; rouchal@utb.cz (M.R.); jhermanova@utb.cz (J.R.) 2 Department of Experimental Biology, Palacký University, Šlechtitelů 27, 783 71 Olomouc, Czech Republic; vladimir.krystof@upol.cz (V.K.); veronika.vojackova@upol.cz (V.V.) 3 Institute of Analytical Chemistry of the Czech Academy of Sciences, Veveří 97, 602 00 Brno, Czech Republic; cmelik@iach.cz * Correspondence: rvicha@utb.cz; Tel.: +420-576-031-103
utb.fulltext.dates	Received: 31 October 2021 Accepted: 22 November 2021 Published: 24 November 2021
utb.fulltext.sponsorship	This research was funded by the Internal Funding Agency of the Tomas Bata University in Zlín (IGA/FT/2021/001), the Czech Science Foundation (GA 19-08410S) and the Institute of Analytical Chemistry of the Czech Academy of Sciences (RVO: 68081715).
utb.wos.affiliation	[Rouchal, Michal; Rudolfova, Jana; Vicha, Robert] Tomas Bata Univ Zlin, Fac Technol, Dept Chem, Vavreckova 275, Zlin 76001, Czech Republic; [Krystof, Vladimir; Vojackova, Veronika] Palacky Univ, Dept Expt Biol, Slechtitelu 27, Olomouc 78371, Czech Republic; [Cmelik, Richard] Czech Acad Sci, Inst Analyt Chem, Veveri 97, Brno 60200, Czech Republic
utb.scopus.affiliation	Department of Chemistry, Faculty of Technology, Tomas Bata University in Zlín, Vavrečkova 275, Zlín, 760 01, Czech Republic; Department of Experimental Biology, Palacký University, Šlechtitelů 27, Olomouc, 783 71, Czech Republic; Institute of Analytical Chemistry of the Czech Academy of Sciences, Veveří 97, Brno, 602 00, Czech Republic
utb.fulltext.projects	IGA/FT/2021/001
utb.fulltext.projects	GA 19-08410S
utb.fulltext.projects	68081715
utb.fulltext.faculty	Faculty of Technology
utb.fulltext.ou	Department of Chemistry