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Dive into the research topics where Lubica Kalachova is active.

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Featured researches published by Lubica Kalachova.


Molecules | 2014

Inhibition of GlcNAc-Processing Glycosidases by C-6-Azido-NAG-Thiazoline and Its Derivatives

Jana Krejzová; Petr Šimon; Lubica Kalachova; Natallia Kulik; Pavla Bojarová; Petr Marhol; Helena Pelantová; Josef Cvačka; Rüdiger Ettrich; Kristýna Slámová; Vladimír Křen

NAG-thiazoline is a strong competitive inhibitor of GH20 β-N-acetyl- hexosaminidases and GH84 β-N-acetylglucosaminidases. Here, we focused on the design, synthesis and inhibition potency of a series of new derivatives of NAG-thiazoline modified at the C-6 position. Dimerization of NAG-thiazoline via C-6 attached triazole linkers prepared by click chemistry was employed to make use of multivalency in the inhibition. Novel compounds were tested as potential inhibitors of β-N-acetylhexosaminidases from Talaromyces flavus, Streptomyces plicatus (both GH20) and β-N-acetylglucosaminidases from Bacteroides thetaiotaomicron and humans (both GH84). From the set of newly prepared NAG-thiazoline derivatives, only C-6-azido-NAG-thiazoline displayed inhibition activity towards these enzymes; C-6 triazole-substituted NAG-thiazolines lacked inhibition activity against the enzymes used. Docking of C-6-azido-NAG-thiazoline into the active site of the tested enzymes was performed. Moreover, a stability study with GlcNAc-thiazoline confirmed its decomposition at pH < 6 yielding 2-acetamido-2-deoxy-1-thio-α/β-D-glucopyranoses, which presumably dimerize oxidatively into S-S linked dimers; decomposition products of NAG-thiazoline are void of inhibitory activity.


Bioorganic & Medicinal Chemistry Letters | 2014

Inhibition of microbial β-N-acetylhexosaminidases by 4-deoxy- and galacto-analogues of NAG-thiazoline.

Jana Krejzová; Lubica Kalachova; Petr Šimon; Helena Pelantová; Kristýna Slámová; Vladimír Křen

NAG-thiazoline is a well-established competitive inhibitor of two physiologically relevant glycosidase families-β-N-acetylhexosaminidases (GH20) and β-N-acetylglucosaminidases (GH84). Based on the different substrate flexibilities of these enzyme groups, we designed and synthesized the 4-deoxy derivative of NAG-thiazoline aiming at the selective inhibition of GH20 β-N-acetylhexosaminidases. One GH84 and two GH20 microbial glycosidases were employed as model enzymes for the inhibition assays. Surprisingly, the new compound 4-deoxy-thiazoline exhibited no activity inhibition with either of the enzyme families of interest. Unlike with the substrates, the 4-hydroxyl group of the inhibitors sugar ring seems to be crucial for binding the inhibitor to the active sites of these enzymes.


Nucleic acids symposium series (2004) | 2008

Novel base-functionalized DNA. Efficient methodology for construction and bioanalytical applications

Michal Hocek; Milan Vrabel; Hana Cahová; Jan Riedl; Lubica Kalachova; Hana Pivoňková; Petra Horáková; Luděk Havran; Miroslav Fojta

A novel efficient two-step methodology for the construction of base-functionalized DNA is based on direct aqueous cross-coupling reactions of unprotected nucleoside triphosphates followed by polymerase incorporation. Preliminary applications of the modified DNA in electrochemical detection and bioanalysis are outlined.


Chemistry: A European Journal | 2009

Base-modified DNA labeled by [Ru(bpy)(3)](2+) and [Os(bpy)(3)](2+) complexes: construction by polymerase incorporation of modified nucleoside triphosphates, electrochemical and luminescent properties, and applications.

Milan Vrabel; Petra Horáková; Hana Pivoňková; Lubica Kalachova; Hana Černocká; Hana Cahová; Radek Pohl; Peter Šebest; Luděk Havran; Michal Hocek; Miroslav Fojta


Organic and Biomolecular Chemistry | 2012

Synthesis of nucleoside mono- and triphosphates bearing oligopyridine ligands, their incorporation into DNA and complexation with transition metals

Lubica Kalachova; Radek Pohl; Michal Hocek


Advanced Synthesis & Catalysis | 2015

Synthesis of Derivatized Chitooligomers using Transglycosidases Engineered from the Fungal GH20 β‐N‐Acetylhexosaminidase

Kristýna Slámová; Jana Krejzová; Petr Marhol; Lubica Kalachova; Natallia Kulik; Helena Pelantová; Josef Cvačka; Vladimír Křen


Organic and Biomolecular Chemistry | 2013

Synthesis of nucleosides and dNTPs bearing oligopyridine ligands linked through an octadiyne tether, their incorporation into DNA and complexation with transition metal cations

Lubica Kalachova; Radek Pohl; Lucie Bednárová; Jindřich Fanfrlík; Michal Hocek


Synthesis | 2009

Synthesis of 2′-Deoxyuridineand 2′-Deoxycytidine Nucleosides Bearing Bipyridineand Terpyridine Ligands at Position 5

Lubica Kalachova; Radek Pohl; Michal Hocek


Collection of Czechoslovak Chemical Communications | 2011

Synthesis of nucleotides bearing oligopyridine ligands and their incorporation into DNA

Lubica Kalachova; Michal Hocek


Collection of Czechoslovak Chemical Communications | 2011

Polymerase construction of base-modified DNA for chemical biology

Michal Hocek; Hana Macíčková-Cahová; Pavel Kielkowski; Veronika Raindlová; Lubica Kalachova; Jan Riedl; Jana Balintová; Petra Ménová

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Michal Hocek

Charles University in Prague

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Radek Pohl

Academy of Sciences of the Czech Republic

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Helena Pelantová

Academy of Sciences of the Czech Republic

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Jana Krejzová

Academy of Sciences of the Czech Republic

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Kristýna Slámová

Academy of Sciences of the Czech Republic

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Vladimír Křen

Academy of Sciences of the Czech Republic

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Hana Cahová

Academy of Sciences of the Czech Republic

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Hana Pivoňková

Academy of Sciences of the Czech Republic

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Jan Riedl

Academy of Sciences of the Czech Republic

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Josef Cvačka

Academy of Sciences of the Czech Republic

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