Your search keyword '"Marie Vajrychová"' showing total 8 results

1. Impact of anesthetics on rat hippocampus and neocortex: A comprehensive proteomic study based on label-free mass spectrometry

Author

David Astapenko, Marie Vajrychova, Ivo Fabrik, Rudolf Kupcik, Kristyna Pimkova, Vojtech Tambor, Vera Radochova, and Vladimir Cerny

Subjects

Label-free proteomics, Anesthetics, Neocortex, Hippocampus, Long-term potentiation, NMDAR, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Anesthesia is regarded as an important milestone in medicine. However, the negative effect on memory and learning has been observed. In addition, the impact of anesthetics on postoperative cognitive functions is still discussed. In this work, in vivo experiment simulating a general anesthesia and ICU sedation was designed to assess the impact of two intravenous (midazolam, dexmedetomidine) and two inhalational (isoflurane, desflurane) agents on neuronal centers for cognition (neocortex), learning, and memory (hippocampus). More than 3600 proteins were quantified across both neocortex and hippocampus. Proteomic study revealed relatively mild effects of anesthetics, nevertheless, protein dysregulation uncovered possible different effect of isoflurane (and midazolam) compared to desflurane (and dexmedetomidine) to neocortical and hippocampal proteins. Isoflurane induced the upregulation of hippocampal NMDAR and other proteins of postsynaptic density and downregulation of GABA signaling, whereas desflurane and dexmedetomidine rather targeted mitochondrial VDAC isoforms and protein regulating apoptotic activity.

Published

2024

2. Peroxiredoxin 6 protects irradiated cells from oxidative stress and shapes their senescence-associated cytokine landscape

Author

Barbora Salovska, Alexandra Kondelova, Kristyna Pimkova, Zuzana Liblova, Miroslav Pribyl, Ivo Fabrik, Jiri Bartek, Marie Vajrychova, and Zdenek Hodny

Subjects

Cellular senescence, Interleukin 6, Peroxiredoxin 6, Redox proteomics, Senescence-associated secretory phenotype, SILAC-iodoTMT, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Cellular senescence is a complex stress response defined as an essentially irreversible cell cycle arrest mediated by the inhibition of cell cycle-specific cyclin dependent kinases. The imbalance in redox homeostasis and oxidative stress have been repeatedly observed as one of the hallmarks of the senescent phenotype. However, a large-scale study investigating protein oxidation and redox signaling in senescent cells in vitro has been lacking. Here we applied a proteome-wide analysis using SILAC-iodoTMT workflow to quantitatively estimate the level of protein sulfhydryl oxidation and proteome level changes in ionizing radiation-induced senescence (IRIS) in hTERT-RPE-1 cells. We observed that senescent cells mobilized the antioxidant system to buffer the increased oxidation stress. Among the antioxidant proteins with increased relative abundance in IRIS, a unique 1-Cys peroxiredoxin family member, peroxiredoxin 6 (PRDX6), was identified as an important contributor to protection against oxidative stress. PRDX6 silencing increased ROS production in senescent cells, decreased their resistance to oxidative stress-induced cell death, and impaired their viability. Subsequent SILAC-iodoTMT and secretome analysis after PRDX6 silencing showed the downregulation of PRDX6 in IRIS affected protein secretory pathways, decreased expression of extracellular matrix proteins, and led to unexpected attenuation of senescence-associated secretory phenotype (SASP). The latter was exemplified by decreased secretion of pro-inflammatory cytokine IL-6 which was also confirmed after treatment with an inhibitor of PRDX6 iPLA2 activity, MJ33. In conclusion, by combining different methodological approaches we discovered a novel role of PRDX6 in senescent cell viability and SASP development. Our results suggest PRDX6 could have a potential as a drug target for senolytic or senomodulatory therapy.

Published

2022

3. Quantification of cellular protein and redox imbalance using SILAC-iodoTMT methodology

Author

Marie Vajrychova, Barbora Salovska, Kristyna Pimkova, Ivo Fabrik, Vojtech Tambor, Alexandra Kondelova, Jiri Bartek, and Zdenek Hodny

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Under normal conditions, the cellular redox status is maintained in a steady state by reduction and oxidation processes. These redox alterations in the cell are mainly sensed by protein thiol residues of cysteines thus regulating protein function. The imbalance in redox homeostasis may therefore regulate protein turnover either directly by redox modulating of transcription factors or indirectly by the degradation of damaged proteins due to oxidation. A new analytical method capable of simultaneously assessing cellular protein expression and cysteine oxidation would provide a valuable tool for the field of cysteine-targeted biology. Here, we show a workflow based on protein quantification using metabolic labeling and determination of cysteine oxidation using reporter ion quantification. We applied this approach to determine protein and redox changes in cells after 5-min, 60-min and 32-h exposure to H2O2, respectively. Based on the functional analysis of our data, we confirmed a biological relevance of this approach and its applicability for parallel mapping of cellular proteomes and redoxomes under diverse conditions. In addition, we revealed a specific pattern of redox changes in peroxiredoxins in a short time-interval cell exposure to H2O2. Overall, our present study offers an innovative, versatile experimental approach to the multifaceted assessment of cellular proteome and its redox status, with broad implications for biomedical research towards a better understanding of organismal physiology and diverse disease conditions. Keywords: SILAC-iodoTMT labeling, Proteome, Redoxome, Cysteine, Liquid chromatography/mass spectrometry, Peroxiredoxin

Published

2019

4. Proteomic Analysis of Early Mid-Trimester Amniotic Fluid Does Not Predict Spontaneous Preterm Delivery.

Author

Maria Hallingström, Juraj Lenco, Marie Vajrychova, Marek Link, Vojtech Tambor, Victor Liman, Maria Bullarbo, Staffan Nilsson, Panagiotis Tsiartas, Teresa Cobo, Marian Kacerovsky, and Bo Jacobsson

Subjects

Medicine, Science

Abstract

OBJECTIVE:The aim of this study was to identify early proteomic biomarkers of spontaneous preterm delivery (PTD) in mid-trimester amniotic fluid from asymptomatic women. METHODS:This is a case-cohort study. Amniotic fluid from mid-trimester genetic amniocentesis (14-19 weeks of gestation) was collected from 2008 to 2011. The analysis was conducted in 24 healthy women with subsequent spontaneous PTD (cases) and 40 randomly selected healthy women delivering at term (controls). An exploratory phase with proteomics analysis of pooled samples was followed by a verification phase with ELISA of individual case and control samples. RESULTS:The median (interquartile range (IQR: 25th; 75th percentiles) gestational age at delivery was 35+5 (33+6-36+6) weeks in women with spontaneous PTD and 40+0 (39+1-40+5) weeks in women who delivered at term. In the exploratory phase, the most pronounced differences were found in C-reactive protein (CRP) levels, that were approximately two-fold higher in the pooled case samples than in the pooled control samples. However, we could not verify these differences with ELISA. The median (25th; 75th IQR) CRP level was 95.2 ng/mL (64.3; 163.5) in women with spontaneous PTD and 86.0 ng/mL (51.2; 145.8) in women delivering at term (p = 0.37; t-test). CONCLUSIONS:Proteomic analysis with mass spectrometry of mid-trimester amniotic fluid suggests CRP as a potential marker of spontaneous preterm delivery, but this prognostic potential was not verified with ELISA.

Published

2016

5. Mid-trimester amniotic fluid proteome's association with spontaneous preterm delivery and gestational duration.

Author

Maria Hallingström, Petra Zedníková, Vojtěch Tambor, Malin Barman, Marie Vajrychová, Juraj Lenčo, Felicia Viklund, Linda Tancred, Hardis Rabe, Daniel Jonsson, Alisa Kachikis, Staffan Nilsson, Marian Kacerovský, Kristina M Adams Waldorf, and Bo Jacobsson

Subjects

Medicine, Science

Abstract

BACKGROUND:Amniotic fluid is clinically accessible via amniocentesis and its protein composition may correspond to birth timing. Early changes in the amniotic fluid proteome could therefore be associated with the subsequent development of spontaneous preterm delivery. OBJECTIVE:The main objective of this study was to perform unbiased proteomics analysis of the association between mid-trimester amniotic fluid proteome and spontaneous preterm delivery and gestational duration, respectively. A secondary objective was to validate and replicate the findings by enzyme-linked immunosorbent assay using a second independent cohort. METHODS:Women undergoing a mid-trimester genetic amniocentesis at Sahlgrenska University Hospital/Östra between September 2008 and September 2011 were enrolled in this study, designed in three analytical stages; 1) an unbiased proteomic discovery phase using LC-MS analysis of 22 women with subsequent spontaneous preterm delivery (cases) and 37 women who delivered at term (controls), 2) a validation phase of proteins of interest identified in stage 1, and 3) a replication phase of the proteins that passed validation using a second independent cohort consisting of 20 cases and 40 matched controls. RESULTS:Nine proteins were nominally significantly associated with both spontaneous preterm delivery and gestational duration, after adjustment for gestational age at sampling, but none of the proteins were significant after correction for multiple testing. Several of these proteins have previously been described as being associated with spontaneous PTD etiology and six of them were thus validated using enzyme linked immunosorbent assay. Two of the proteins passed validation; Neutrophil gelatinase-associated lipocalin and plasminogen activator inhibitor 1, but the results could not be replicated in a second cohort. CONCLUSIONS:Neutrophil gelatinase-associated lipocalin and Plasminogen activator inhibitor 1 are potential biomarkers of spontaneous preterm delivery and gestational duration but the findings could not be replicated. The negative findings are supported by the fact that none of the nine proteins from the exploratory phase were significant after correction for multiple testing.

Published

2020

6. OPCW BIOMEDICAL PROFICIENCY TEST IN THE LABORATORY OF ANALYTICAL CHEMISTRY AT THE DEPARTMENT OF TOXICOLOGY AND MILITARY PHARMACY

Author

Rafael Doležal, David Herman, Petr Bzonek, Lukáš Prchal, Marie Vajrychová, Nela Váňová, Alžběta Dlabková, and Daniel Jun

Subjects

Emergency Medical Services, Immunology and Microbiology (miscellaneous), Veterinary (miscellaneous), Public Health, Environmental and Occupational Health, Emergency Medicine, Pharmacology, Toxicology and Pharmaceutics (miscellaneous)

Abstract

S ohledem na udalosti poslednich let neni riziko vojenskeho ci teroristickeho zneužiti vysoce toxických latek vcetně zakazaných bojových otravných latek zanedbatelne. Katedra toxikologie a vojenske farmacie Fakulty vojenskeho zdravotnictvi Univerzity obrany tudiž zavedla analyticke metody a postupy uprav biologických vzorků (plasma, moc) pro stanoveni identifikacnich znaků (biomarkerů) vystaveni nervově paralytickým latkam (sarinu, cyklosarinu, somanu, tabunu a V-latkam) a yperitu, cimž přinasi do Armady Ceske republiky schopnost potvrdit jejich zneužiti vůci žive sile. Metody popsane v clanku jsou založeny na průkazu metabolitů (O-alkyl methylfosfonových kyselin pro nervově paralyticke latky a thiodiglykolu pro yperit) a produktů jejich reakci s přitomnými biomolekulami (tyrosinových aduktů nervově paralytických latek a peptidových aduktů sirneho yperitu) pomoci kapalinove a plynove chromatografie spojene s hmotnostni spektrometrii. Funkcnost těchto metod je ověřovana a diskutovana v ramci testu odborne způsobilosti pro biomedicinskou analýzu s mezinarodni ucasti, který každorocně pořada Organizace pro zakaz chemických zbrani. Katedra se těchto testů ucastni od roku 2016, kdy se konal prvni rocnik.

Published

2020

7. Mid-trimester amniotic fluid proteome’s association with spontaneous preterm delivery and gestational duration

Author

Alisa Kachikis, Juraj Lenčo, Petra Zedníková, Malin Barman, Bo Jacobsson, Linda Tancred, Vojtěch Tambor, Hardis Rabe, Staffan Nilsson, Kristina M. Adams Waldorf, Maria Hallingström, Daniel Jonsson, Marie Vajrychová, Marian Kacerovský, and Felicia Viklund

Subjects

Proteomics, Male, Amniotic fluid, infekce, Proteome, Physiology, Proteomes, Maternal Health, labor, multiple proteins, microbial invasion, Pathology and Laboratory Medicine, Biochemistry, Cohort Studies, chemistry.chemical_compound, Labor and Delivery, Pregnancy, Prenatal Diagnosis, biomarker discovery, Medicine and Health Sciences, Enzyme-Linked Immunoassays, Immune Response, Multidisciplinary, medicine.diagnostic_test, Obstetrics, Gestational age, Obstetrics and Gynecology, Body Fluids, mikrobiální invaze, Obstetric Procedures, Plasminogen activator inhibitor-1, Pregnancy Trimester, Second, Cohort, Amniocentesis, Gestation, Medicine, Premature Birth, Female, women, zánět, ženy, Anatomy, lipocalin asociovaný s želatinázou, Cohort study, Research Article, Adult, medicine.medical_specialty, objev biomarkerů, Science, Immunology, předpověď, předčasné prasknutí, Surgical and Invasive Medical Procedures, Gestational Age, Preterm Birth, Research and Analysis Methods, gelatinase-associated lipocalin, více proteinů, Signs and Symptoms, Diagnostic Medicine, medicine, práce, Humans, Immunoassays, Inflammation, business.industry, premature rupture, Biology and Life Sciences, Proteins, prediction, medicine.disease, Amniotic Fluid, infection, Pregnancy Complications, chemistry, inflammation, Birth, Immunologic Techniques, Women's Health, business

Abstract

Background Amniotic fluid is clinically accessible via amniocentesis and its protein composition may correspond to birth timing. Early changes in the amniotic fluid proteome could therefore be associated with the subsequent development of spontaneous preterm delivery. Objective The main objective of this study was to perform unbiased proteomics analysis of the association between mid-trimester amniotic fluid proteome and spontaneous preterm delivery and gestational duration, respectively. A secondary objective was to validate and replicate the findings by enzyme-linked immunosorbent assay using a second independent cohort. Methods Women undergoing a mid-trimester genetic amniocentesis at Sahlgrenska University Hospital/Ostra between September 2008 and September 2011 were enrolled in this study, designed in three analytical stages; 1) an unbiased proteomic discovery phase using LC-MS analysis of 22 women with subsequent spontaneous preterm delivery (cases) and 37 women who delivered at term (controls), 2) a validation phase of proteins of interest identified in stage 1, and 3) a replication phase of the proteins that passed validation using a second independent cohort consisting of 20 cases and 40 matched controls. Results Nine proteins were nominally significantly associated with both spontaneous preterm delivery and gestational duration, after adjustment for gestational age at sampling, but none of the proteins were significant after correction for multiple testing. Several of these proteins have previously been described as being associated with spontaneous PTD etiology and six of them were thus validated using enzyme linked immunosorbent assay. Two of the proteins passed validation; Neutrophil gelatinase-associated lipocalin and plasminogen activator inhibitor 1, but the results could not be replicated in a second cohort. Conclusions Neutrophil gelatinase-associated lipocalin and Plasminogen activator inhibitor 1 are potential biomarkers of spontaneous preterm delivery and gestational duration but the findings could not be replicated. The negative findings are supported by the fact that none of the nine proteins from the exploratory phase were significant after correction for multiple testing. Dosavadní výzkum Plodová voda je klinicky přístupná prostřednictvím amniocentézy a její proteinové složení může odpovídat načasování porodu. Časné změny v proteomu plodové vody by proto mohly být spojeny s následným vývojem spontánního předčasného porodu. Cíl Hlavním cílem této studie bylo provést objektivní proteomickou analýzu asociace mezi proteomem plodové vody ve středním trimestru a spontánním předčasným porodem, respektive gestační dobou. Sekundárním cílem bylo ověřit a replikovat nálezy pomocí enzymového imunosorbentního testu s použitím druhé nezávislé kohorty. Metody Do této studie, která byla koncipována ve třech analytických fázích, byly zařazeny ženy podstupující genetickou amniocentézu v polovině trimestru ve Fakultní nemocnici Sahlgrenska / Ostra v období od září 2008 do září 2011; 1) nezaujatá fáze proteomického objevu pomocí LC-MS analýzy 22 žen s následným spontánním předčasným porodem (případy) a 37 žen, které porodily v termínu (kontroly), 2) ověřovací fáze sledovaných proteinů identifikovaných ve stadiu 1 a 3 ) replikační fáze proteinů, která prošla validací pomocí druhé nezávislé kohorty skládající se z 20 případů a 40 shodných kontrol. Výsledky Devět proteinů bylo nominálně významně spojeno jak se spontánním předčasným porodem, tak s gestačním trváním po úpravě na gestační věk při odběru vzorků, ale žádný z proteinů nebyl významný po korekci na vícenásobné testování. Některé z těchto proteinů byly dříve popsány jako asociované se spontánní etiologií PTD a šest z nich bylo tedy validováno pomocí enzymového imunosorbentního testu. Dva z proteinů prošly validací; Lipokalin spojený s neutrofilní gelatinázou a inhibitor aktivátoru plazminogenu 1, ale výsledky nemohly být replikovány ve druhé kohortě. Závěry Lipokalin spojený s neutrofilní gelatinázou a inhibitor aktivátoru plazminogenu 1 jsou potenciálními biomarkery spontánního předčasného porodu a gestačního trvání, ale nálezy nelze replikovat. Negativní zjištění podporuje skutečnost, že žádný z devíti proteinů z průzkumné fáze nebyl významný po korekci na vícenásobné testování.

Published

2020

8. Conventional-Flow Liquid Chromatography-Mass Spectrometry for Exploratory Bottom-Up Proteomic Analyses.

Author

Juraj Lenčo, Marie Vajrychová, Pimková, Kristýna, Prokšová, Magdaléna, Benková, Markéta, Klimentová, Jana, Tambor, Vojtěch, and Soukup, Ondřej

Subjects

*LIQUID chromatography-mass spectrometry, *PROTEOMICS, *PEPTIDES, *FORMIC acid, *DIMETHYL sulfoxide, *MASS spectrometry

Abstract

Due to its sensitivity and productivity, bottom-up proteomics based on liquid chromatography-mass spectrometry (LC-MS) has become the core approach in the field. The de facto standard LC-MS platform for proteomics operates at sub-µL/min flow rates, and nanospray is required for efficiently introducing peptides into a mass spectrometer. Although this is almost a "dogma", this view is being reconsidered in light of developments in highly efficient chromatographic columns, and especially with the introduction of exceptionally sensitive MS instruments. Although conventional-flow LC-MS platforms have recently penetrated targeted proteomics successfully, their possibilities in discovery-oriented proteomics have not yet been thoroughly explored. Our objective was to determine what are the extra costs and what optimization and adjustments to a conventional-flow LC-MS system must be undertaken to identify a comparable number of proteins as can be identified on a nanoLC-MS system. We demonstrate that the amount of a complex tryptic digest needed for comparable proteome coverage can be roughly 5-fold greater, providing the column dimensions are properly chosen, extra-column peak dispersion is minimized, column temperature and flow rate are set to levels appropriate for peptide separation, and the composition of mobile phases is fine-tuned. Indeed, we identified 2 835 proteins from 2 µg of HeLa cells tryptic digest separated during a 60 min gradient at 68 µL/min on a 1.0 mm x 250 mm column held at 55 °C and using an aqua-acetonitrile mobile phases containing 0.1% formic acid, 0.4% acetic acid, and 3% dimethyl sulfoxide. Our results document that conventional-flow LC-MS is an attractive alternative for bottom-up exploratory proteomics. [ABSTRACT FROM AUTHOR]

Published

2018