Tomáš Parák scite author profile

Tomáš Parák

4Publications

74Citation Statements Received

43Citation Statements Given

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Affiliations

Masaryk University, University of Veterinary Sciences Brno, Hospital of the Brothers of St. John of God

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Activity of Na+/K+-activated Mg2+-dependent ATP-hydrolase in the cell-free extracts of the sulfate-reducing bacteria Desulfovibrio piger Vib-7 and Desulfomicrobium sp. Rod-9

et al. 2015

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The aim of our work was to study Na -dependent ATPase activity in cellfree extracts of the sulfate-reducing bacteria Desulfovibrio piger Vib-7 and Desulfomicrobium sp. Rod-9 isolated from the human large intestine, and to carry out the kinetic analysis of the enzyme reaction. The maximum ATPase activity for both bacterial strains at +35 ºC was determined. The highest activities of the studied enzyme in the cell-free extracts of D. piger Vib-7 at pH 7.0 and Desulfomicrobium sp. Rod-9 at pH 6.5 were measured. Based on experimental data, the analysis of kinetic properties of the ATP-hydrolase reaction by the studied bacteria was carried out. The enzyme activity, initial (instantaneous) reaction rate (V 0 ) and maximum rate of the ATPase reaction (V max ) was significantly higher in D. piger Vib-7 cells than in Desulfomicrobium sp. Rod-9. Michaelis constants (K m ) of the enzyme reaction for both bacterial strains were determined. ATPase activity, hydrogen sulfide, intestinal microbiocenosis, bowel diseases, ulcerative colitisSulfate-reducing bacteria carry out the dissimilatory sulfate reduction during anaerobic respiration (Barton and Hamilton 2007). The final product of the sulfate reduction in the human intestine is hydrogen sulfide which is carcinogenic to its cells, and can cause inhibition of cytochrome oxidase, colonocytes oxidation of butyrate, destruction of epithelial cells, development of ulcers, and inflammation with subsequent development of colon cancer (Pitcher and Cummings 1996;Gibson et al. 1991;Cummings et al. 2003). The transport of sulfate ions and organic compounds in the cytoplasm of the bacterial cells occurs through active transport using ATP energy (Barton and Hamilton 2007). In this regard, it is very important to study the mechanisms of sulfate ions transport, enzymatic activity and kinetic properties of other ATP-dependent enzymes of sulfatereducing bacteria from human intestine.Plentiful data are available on the functions of biological membranes including the integral membrane protein ATP-dependent systems of transport ions (Lodish et al. 2000;Yuan et al. 2005;Tian et al. 2006). However, the ATPase activity of the sulfate-reducing bacteria Desulfovibrio piger and Desulfomicrobium sp. isolated from the human large intestine has not been studied yet. A comprehensive study of the functioning and role of Na + /K + -pump as a system of energy-dependent transport of different ions in the regulation of the dissimilatory sulfate reduction and accumulation of hydrogen sulfide will enable to form a holistic view on the participation of these systems in maintaining ion homeostasis of the sulfate-reducing bacteria cells.The aim of our work was to study Na-dependent ATPase activity in cell-free extracts of the sulfate-reducing bacteria Desulfovibrio piger Vib-7 and Desulfomicrobium sp. Rod-9 isolated from the human large intestine, and to carry out the kinetic analysis of the enzyme reaction.

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Hepatoprotective and proapoptotic effect of Ecballium elaterium on CCl4-induced hepatotoxicity in rats

Naggar

Chalupová

Pražanová

et al. 2015

Asian Pacific Journal of Tropical Medicine

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Nilotinib Induces ER Stress and Cell Death in H9c2 Cells

Lekeš

Szadvári²,

Križanová³

et al. 2016

Physiol Res

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Tyrosine kinases inhibitors (TKi) represent a relatively novel class of anticancer drugs that target cellular pathways overexpressed in certain types of malignancies, such as chronic myeloid leukaemia (CML). Nilotinib, ponatinib and imatinib exhibit cardiotoxic and vascular effects. In this study, we focused on possible cardiotoxicity of nilotinib using H9c2 cells as a suitable cell model. We studied role of endoplasmic reticulum (ER) stress and apoptosis in nilotinib toxicity using a complex approach. Nilotinib impaired mitochondrial function and induced formation of ROS under clinically relevant concentrations. In addition, ability of nilotinib to induce ER stress has been shown. These events result in apoptotic cell death. All these mechanisms contribute to cytotoxic effect of the drug. In addition, involvement of ER stress in nilotinib toxicity may be important in co-treatment with pharmaceuticals affecting ER and ER stress, e.g. beta-blockers or sartans, and should be further investigated.

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Zinc as a feed supplement and its impact on plasma cholesterol concentrations in breeding cocks

Parák

Straková

2011

Acta Vet. Brno

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Tomáš Parák

Activity of Na+/K+-activated Mg2+-dependent ATP-hydrolase in the cell-free extracts of the sulfate-reducing bacteria Desulfovibrio piger Vib-7 and Desulfomicrobium sp. Rod-9

Hepatoprotective and proapoptotic effect of Ecballium elaterium on CCl4-induced hepatotoxicity in rats

Nilotinib Induces ER Stress and Cell Death in H9c2 Cells

Zinc as a feed supplement and its impact on plasma cholesterol concentrations in breeding cocks

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