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Archive | 1999

Synthetic Cyclin Dependent Kinase Inhibitors

Marian Hajduch; Libor Havlíèek; Jaroslav Veselý; Radko Novotný; Vladimír Mihál; Miroslav Strnad

The unsatisfactory results of current anti-cancer therapies require the active search for new drugs, new treatment strategies and a deeper understanding of the host-tumour relationship. From this point of view, the drugs with a capacity to substitute the functions of altered tumour suppressor genes are of prominent interest. Since one of the main functions of onco-suppressors is to mediate cell cycle arrest via modification of cyclin dependent kinases (CDKs) activity, the compounds with ability to substitute altered functions of these genes in neoplastic cells are of prominent interest. Synthetic inhibitors of cyclin dependent kinases (CDKIs) are typical representatives of such drugs. Olomoucine (OC), flavopiridol (FP), butyrolactone I (BL) and their derivatives selectively inhibit CDKs and thus constrain tumor cell proliferation under in vitro and/or in vivo conditions. We originally discovered OC and its inhibitory activity toward CDK1 family of CDKs, and recently reported the induction of apoptosis and tumor regression following OC application. Moreover, the OC family of synthetic CDKIs has the capacity to directly inhibit CDK7, the principal enzyme required for activating other CDKs, and thus these compounds are the first known CDK7 inhibitors. Its unique mechanism of action and potent anti-cancer activity under both in vitro and in vivo conditions provide a unique tool to inhibit tumour cell proliferation, and to selectively induce apoptosis in neoplastic tissues. The mechanisms of anti-cancer activities of FP, BL, OC and related synthetic CDKIs are compared and discussed in this paper.


FEBS Journal | 1994

Inhibition of Cyclin‐Dependent Kinases by Purine Analogues

Jaroslav Veselý; Libor Havlíček; Miroslav Strnad; J. Julian Blow; Arianna Donella-Deana; Lorenzo A. Pinna; D. S. Letham; Jun-ya Kato; Lénaïck Détivaud; Sophie Leclerc; Laurent Meijer


Journal of Medicinal Chemistry | 1997

Cytokinin-Derived Cyclin-Dependent Kinase Inhibitors: Synthesis and cdc2 Inhibitory Activity of Olomoucine and Related Compounds

Libor Havlíček; Jan Hanuš; Jaroslav Veselý; Sophie Leclerc; Laurent Meijer; Gordon Shaw; Miroslav Strnad


Archive | 2000

Substituted nitrogen heterocyclic derivatives and pharmaceutical use thereof

Jan Hanuš; Vladimír Kryštof; Marian Hajduch; Jaroslav Veselý; Miroslav Strnad


Advances in Experimental Medicine and Biology | 1999

Synthetic cyclin dependent kinase inhibitors. New generation of potent anti-cancer drugs.

Marian Hajduch; Havlíèek L; Jaroslav Veselý; Novotný R; Mihál; Miroslav Strnad


Drug Metabolism and Disposition | 2001

In Vivo Metabolism of 2,6,9-Trisubstituted Purine-Derived Cyclin-Dependent Kinase Inhibitor Bohemine in Mice: Glucosidation as the Principal Metabolic Route

Zdeněk Chmela; Jaroslav Veselý; Karel Lemr; Miroslav Rypka; Jan Hanuš; Libor Havlíček; Vladimír Kryštof; Lucie Michnová; Květoslava Fuksová; Jiřı́ Lukeš


Biomedical papers of the Medical Faculty of the University Palacky, Olomouc, Czechoslovakia | 2001

CELL SUSPENSIONS, CELL CULTURES, AND TISSUE SLICES – IMPORTANT METABOLIC IN VITRO SYSTEMS

Kateřina Červenková; Marie Belejova; Jaroslav Veselý; Zdeněk Chmela; Miroslav Rypka; Jitka Ulrichová; Martin Modrianský; Patrick Maurel


Cryobiology | 2006

A novel simplified ultra-rapid freezing technique for cryopreservation of tissue slices

Miroslav Rypka; Kateřina Červenková; Lenka Uherková; Hana Poczatková; Anthony V. Florschutz; Jaroslav Veselý


Biomedical papers of the Medical Faculty of the University Palacky, Olomouc, Czechoslovakia | 2005

CHANGES IN mRNA LEVELS OF INTRACELLULAR FATTY ACID METABOLISM REGULATORS IN HUMAN HEPATOMA HepG2 CELLS FOLLOWING THEIR TREATMENT WITH NON-ESTERIFIED FATTY ACIDS AND DEHYDROEPIANDROSTERONE

Miroslav Rypka; Kateřina Červenková; Lenka Uherková; Hana Poczatková; Kateřina Bogdanová; Jaroslav Veselý


Acta Biochimica Polonica | 2010

Evidence for differential effects of glucose and cycloheximide on mRNA levels of peroxisome proliferator-activated receptor- (PPAR-) machinery members: Superinduction of PPAR-γ1 and -γ2 mRNAs

Miroslav Rypka; Jaroslav Veselý

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Jan Hanuš

Academy of Sciences of the Czech Republic

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Libor Havlíček

Academy of Sciences of the Czech Republic

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Laurent Meijer

Centre national de la recherche scientifique

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Sophie Leclerc

Centre national de la recherche scientifique

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Libor Havlíèek

Charles University in Prague

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Lénaïck Détivaud

Centre national de la recherche scientifique

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