Milada Dvořáčková
Masaryk University
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Publication
Featured researches published by Milada Dvořáčková.
Molecules | 2013
Silvie Bernatová; Ota Samek; Zdeněk Pilát; Mojmír Šerý; Jan Ježek; Petr Jákl; Martin Šiler; Vladislav Krzyžánek; Pavel Zemánek; Veronika Holá; Milada Dvořáčková; Filip Růžička
Antibiotics cure infections by influencing bacterial growth or viability. Antibiotics can be divided to two groups on the basis of their effect on microbial cells through two main mechanisms, which are either bactericidal or bacteriostatic. Bactericidal antibiotics kill the bacteria and bacteriostatic antibiotics suppress the growth of bacteria (keep them in the stationary phase of growth). One of many factors to predict a favorable clinical outcome of the potential action of antimicrobial chemicals may be provided using in vitro bactericidal/bacteriostatic data (e.g., minimum inhibitory concentrations—MICs). Consequently, MICs are used in clinical situations mainly to confirm resistance, and to determine the in vitro activities of new antimicrobials. We report on the combination of data obtained from MICs with information on microorganisms’ “fingerprint” (e.g., DNA/RNA, and proteins) provided by Raman spectroscopy. Thus, we could follow mechanisms of the bacteriostatic versus bactericidal action simply by detecting the Raman bands corresponding to DNA. The Raman spectra of Staphylococcus epidermidis treated with clindamycin (a bacteriostatic agent) indeed show little effect on DNA which is in contrast with the action of ciprofloxacin (a bactericidal agent), where the Raman spectra show a decrease in strength of the signal assigned to DNA, suggesting DNA fragmentation.
Analytical Chemistry | 2014
Marie Horká; Pavel Karásek; Filip Růžička; Milada Dvořáčková; Martina Sittová; Michal Roth
Identification and prevention of Staphylococcus aureus-caused infections may benefit from a fast and dependable method to distinguish between the methicillin-resistant (MRSA) and methicillin-susceptible (MSSA) S. aureus strains. The current methods involving polymerase chain reaction and/or other molecular tests are usually laborious and time-consuming. We describe here a fast and low-cost method employing capillary zone electrophoresis (CZE) to distinguish between MRSA and MSSA. The method makes use of a supercritical water-treated fused silica capillary, the inner surface of which has subsequently been modified with (3-glycidyloxypropyl)trimethoxysilane. With optimized proportions of suitable additives to the background electrolyte, a CZE separation of MRSA from MSSA may be completed within 12 min. The cells were baseline-resolved, and resolution was determined to be 3.61. The isoelectric points of MSSA and MRSA were found to be the same for both groups of these strains, pI = 3.4.
Folia Microbiologica | 2018
Milada Dvořáčková; Filip Růžička; Martin Benešík; Roman Pantůček; Monika Dvořáková-Heroldová
Staphylococcus aureus may be a highly virulent human pathogen, especially when it is able to form a biofilm, and it is resistant to antibiotic. Infections caused by these bacteria significantly affect morbidity and mortality, primarily in hospitalized patients. Treatment becomes more expensive, more toxic, and prolonged. This is the reason why research on alternative therapies should be one of the main priorities of medicine and biotechnology. A promising alternative treatment approach is bacteriophage therapy. The effect of the anti-staphylococcal bacteriophage preparation Stafal® on biofilm reduction was assessed on nine S. aureus strains using both sonication with subsequent quantification of surviving cells on the catheter surface and evaluation of biofilm reduction in microtiter plates. It was demonstrated that the bacteriophages destroy planktonic cells very effectively. However, to destroy cells embedded in the biofilm effectively requires a concentration at least ten times higher than that provided by the commercial preparation. The catheter disc method (CDM) allowed easier comparison of the effect on planktonic cells and cells in a biofilm than the microtiter plate (MTP) method.
Archive | 2003
Miroslav Votava; Lenka Černohorská; Monika Dvořáková Heroldová; Veronika Holá; Petr Ondrovčík; Filip Růžička; Vladana Woznicová; Ondřej Zahradníček; Leona Mejzlíková; Milada Dvořáčková
Analytical and Bioanalytical Chemistry | 2014
Marie Horká; Marie Vykydalová; Filip Růžička; Jiří Šalplachta; Veronika Holá; Milada Dvořáčková; Anna Kubesová; Karel Šlais
Archive | 2013
Roman Pantůček; Milada Dvořáčková; Martin Benešík; Jiří Doškař; Ivana Mašlaňová; Vladislava Růžičková; Filip Růžička; Marek Moša
Archive | 2014
Milada Dvořáčková; Tereza Peroutková; Filip Růžička
Archive | 2013
Milada Dvořáčková; Filip Růžička; Monika Dvořáková Heroldová; Tereza Janečková
Archive | 2013
Milada Dvořáčková; Filip Růžička; Monika Dvořáková Heroldová
Archive | 2013
Alena Siváková; Filip Růžička; Martina Mahelová; Milada Dvořáčková