Your search keyword '"Daria V. Evsyutina"' showing total 17 results

1. Molecular Basis of the Slow Growth of Mycoplasma hominis on Different Energy Sources

Author

Daria V. Evsyutina, Tatiana A. Semashko, Maria A. Galyamina, Sergey I. Kovalchuk, Rustam H. Ziganshin, Valentina G. Ladygina, Gleb Y. Fisunov, and Olga V. Pobeguts

Subjects

slow growth, antibiotic sensitivity, Mycoplasma hominis, proteomics, thymidine, Microbiology, QR1-502

Abstract

Mycoplasma hominis is an opportunistic urogenital pathogen in vertebrates. It is a non-glycolytic species that produces energy via arginine degradation. Among genital mycoplasmas, M. hominis is the most commonly reported to play a role in systemic infections and can persist in the host for a long time. However, it is unclear how M. hominis proceeds under arginine limitation. The recent metabolic reconstruction of M. hominis has demonstrated its ability to catabolize deoxyribose phosphate to produce ATP. In this study, we cultivated M. hominis on two different energy sources (arginine and thymidine) and demonstrated the differences in growth rate, antibiotic sensitivity, and biofilm formation. Using label-free quantitative proteomics, we compared the proteome of M. hominis under these conditions. A total of 466 proteins were identified from M. hominis, representing approximately 85% of the predicted proteome, while the levels of 94 proteins changed significantly. As expected, we observed changes in the levels of metabolic enzymes. The energy source strongly affects the synthesis of enzymes related to RNA modifications and ribosome assembly. The translocation of lipoproteins and other membrane-associated proteins was also impaired. Our study, the first global characterization of the proteomic switching of M. hominis in arginine-deficiency media, illustrates energy source-dependent control of pathogenicity factors and can help to determine the mechanisms underlying the interaction between the growth rate and fitness of genome-reduced bacteria.

Published

2022

2. Role of DNA modifications in Mycoplasma gallisepticum

Author

Tatiana A. Semashko, Alexander A. Arzamasov, Daria V. Evsyutina, Irina A. Garanina, Daria S. Matyushkina, Valentina G. Ladygina, Olga V. Pobeguts, Gleb Y. Fisunov, and Vadim M. Govorun

Subjects

Medicine, Science

Abstract

The epigenetics of bacteria, and bacteria with a reduced genome in particular, is of great interest, but is still poorly understood. Mycoplasma gallisepticum, a representative of the class Mollicutes, is an excellent model of a minimal cell because of its reduced genome size, lack of a cell wall, and primitive cell organization. In this study we investigated DNA modifications of the model object Mycoplasma gallisepticum and their roles. We identified DNA modifications and methylation motifs in M. gallisepticum S6 at the genome level using single molecule real time (SMRT) sequencing. Only the ANCNNNNCCT methylation motif was found in the M. gallisepticum S6 genome. The studied bacteria have one functional system for DNA modifications, the Type I restriction-modification (RM) system, MgaS6I. We characterized its activity, affinity, protection and epigenetic functions. We demonstrated the protective effects of this RM system. A common epigenetic signal for bacteria is the m6A modification we found, which can cause changes in DNA-protein interactions and affect the cell phenotype. Native methylation sites are underrepresented in promoter regions and located only near the -35 box of the promoter, which does not have a significant effect on gene expression in mycoplasmas. To study the epigenetics effect of m6A for genome-reduced bacteria, we constructed a series of M. gallisepticum strains expressing EGFP under promoters with the methylation motifs in their different elements. We demonstrated that m6A modifications of the promoter located only in the -10-box affected gene expression and downregulated the expression of the corresponding gene.

Published

2022

3. The Dynamics of Mycoplasma gallisepticum Nucleoid Structure at the Exponential and Stationary Growth Phases

Author

Gleb Y. Fisunov, Alexander I. Zubov, Olga V. Pobeguts, Anna M. Varizhuk, Mariya A. Galyamina, Daria V. Evsyutina, Tatiana A. Semashko, Valentin A. Manuvera, Sergey I. Kovalchuk, Rustam K. Ziganshin, Nicolay A. Barinov, Dmitry V. Klinov, and Vadim M. Govorun

Subjects

Mycoplasma gallisepticum, nucleoid, nucleoid-associated proteins, enolase, proteome, Microbiology, QR1-502

Abstract

The structure and dynamics of bacterial nucleoids play important roles in regulating gene expression. Bacteria of class Mollicutes and, in particular, mycoplasmas feature extremely reduced genomes. They lack multiple structural proteins of the nucleoid, as well as regulators of gene expression. We studied the organization of Mycoplasma gallisepticum nucleoids in the stationary and exponential growth phases at the structural and protein levels. The growth phase transition results in the structural reorganization of M. gallisepticum nucleoid. In particular, it undergoes condensation and changes in the protein content. The observed changes corroborate with the previously identified global rearrangement of the transcriptional landscape in this bacterium during the growth phase transition. In addition, we identified that the glycolytic enzyme enolase functions as a nucleoid structural protein in this bacterium. It is capable of non-specific DNA binding and can form fibril-like complexes with DNA.

Published

2021

4. Gene Silencing through CRISPR Interference in Mycoplasmas

Author

Daria V. Evsyutina, Gleb Y. Fisunov, Olga V. Pobeguts, Sergey I. Kovalchuk, and Vadim M. Govorun

Subjects

CRISPRi, mycoplasma, transcription factors, knockdown, Biology (General), QH301-705.5

Abstract

Mycoplasmas are pathogenic, genome-reduced bacteria. The development of such fields of science as system and synthetic biology is closely associated with them. Despite intensive research of different representatives of this genus, genetic manipulations remain challenging in mycoplasmas. Here we demonstrate a single-plasmid transposon-based CRISPRi system for the repression of gene expression in mycoplasmas. We show that selected expression determinants provide a level of dCas9 that does not lead to a significant slow-down of mycoplasma growth. For the first time we describe the proteomic response of genome-reduced bacteria to the expression of exogenous dcas9. The functionality of the resulting vector is confirmed by targeting the three genes coding transcription factors-fur, essential spxA, whiA, and histone-like protein hup1 in Mycoplasma gallisepticum. As a result, the expression level of each gene was decreased tenfold and influenced the mRNA level of predicted targets of transcription factors. To illustrate the versatility of this vector, we performed a knockdown of metabolic genes in a representative member of another cluster of the Mycoplasma genus-Mycoplasma hominis. The developed CRISPRi system is a powerful tool to discover the functioning of genes that are essential, decipher regulatory networks and that can help to identify novel drug targets to control Mycoplasma infections.

Published

2022

5. Data on proteome of Mycoplasma hominis cultivated with arginine or thymidine as a carbon source

Author

Tatiana A. Semashko, Daria V. Evsyutina, Valentina G. Ladygina, Aleksandr I. Zubov, Irina V. Rakovskaya, Sergey I. Kovalchuk, Rustam H. Ziganshin, and Olga V. Pobeguts

Subjects

Mycoplasma hominis, Proteome, Cultivation conditions, Carbon source, Arginine, Thymidine, Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390

Abstract

Mycoplasma hominis is an opportunistic bacterium that can cause acute and chronic infections of the urogenital tract. This bacterium, like all other Mycoplasma species, is characterized by the reduced genome size, and, consequently, reduction of the main metabolic pathways. M. hominis cells cannot effectively use glucose as a carbon and energy source. Therefore, the main pathway of energy metabolism is the arginine dihydrolase pathway. However, several bacteria can use nucleosides as the sole energy source. Biochemical studies using Salmonella typhimurium have shown that three enzymes (thymidine phosphorylase, phosphopentose mutase and deoxyribose-phosphate aldolase) are involved in the thymidine catabolic pathway. All these enzymes are present in M. hominis. For understanding changes in the energy metabolism of M. hominis we performed shotgun proteome analysis of M. hominis cells in liquid medium with arginine or thymidine as a carbon source. LC-MS analysis was performed with an Ultimate 3000 Nano LC System (Thermo Fisher Scientific) coupled to a Q Exactive HF benchtop Orbitrap mass spectrometer (Thermo Fisher Scientific) via a nanoelectrospray source (Thermo Fisher Scientific). Data are available via ProteomeXchange with identifier PXD018714 (https://www.ebi.ac.uk/pride/archive/projects/PXD018714).

Published

2020

6. Propionate Induces Virulent Properties of Crohn’s Disease-Associated Escherichia coli

Author

Olga V. Pobeguts, Valentina G. Ladygina, Daria V. Evsyutina, Artem V. Eremeev, Aleksandr I. Zubov, Daria S. Matyushkina, Peter L. Scherbakov, Daria V. Rakitina, and Gleb Y. Fisunov

Subjects

Crohn’s disease, Crohn’s disease-associated adherent-invasive Escherichia coli, propionic acid, 2D electrophoresis, macrophages, Microbiology, QR1-502

Abstract

Crohn’s disease (CD) is a severe chronic immune-mediated granulomatous inflammatory disease of the gastrointestinal tract. The mechanisms of CD pathogenesis remain obscure. Metagenomic analysis of samples from CD patients revealed that several of them have the elevated level of Escherichia coli with adhesive–invasive phenotype (AIEC). Previously, we isolated an E. coli strain CD isolate ZvL2 from a patient with CD, which features AIEC phenotype. Here, we demonstrate that prolonged growth on propionate containing medium stimulates virulent properties of CD isolate ZvL2, while prolonged growth on glucose reduces these properties to levels indistinguishable from laboratory strain K-12 MG1655. Propionate presence also boosts the ability of CD isolate ZvL2 to penetrate and colonize macrophages. The effect of propionate is reversible, re-passaging of CD isolate on M9 medium supplemented with glucose leads to the loss of its virulent properties. Proteome analysis of CD isolate ZvL2 growth in medium supplemented with propionate or glucose revealed that propionate induces expression porins OmpA and OmpW, transcription factors PhoP and OmpR, and universal stress protein UspE, which were previously found to be important for macrophage colonization by enteropathogenic bacteria.

Published

2020

7. Thymidine utilisation pathway is a novel phenotypic switch of Mycoplasma hominis

Author

Gleb Yu. Fisunov, Olga V. Pobeguts, Valentina G. Ladygina, Alexandr I. Zubov, Mariya A. Galyamina, Sergey I. Kovalchuk, Rustam K. Ziganshin, Daria V. Evsyutina, Daria S. Matyushkina, Ivan O. Butenko, Olga N. Bukato, Vladimir A. Veselovsky, Tatiana A. Semashko, Ksenia M. Klimina, Galina A. Levina, Olga I. Barhatova, and Irina V. Rakovskaya

Subjects

Microbiology (medical), General Medicine, Microbiology

Abstract

Introduction. Mycoplasma hominis is a bacterium belonging to the class Mollicutes . It causes acute and chronic infections of the urogenital tract. The main features of this bacterium are an absence of cell wall and a reduced genome size (517–622 protein-encoding genes). Previously, we have isolated morphologically unknown M. hominis colonies called micro-colonies (MCs) from the serum of patients with inflammatory urogenital tract infection. Hypothesis. MCs are functionally different from the typical colonies (TCs) in terms of metabolism and cell division. Aim. To determine the physiological differences between MCs and TCs of M. hominis and elucidate the pathways of formation and growth of MCs by a comparative proteomic analysis of these two morphological forms. Methodology. LC–MS proteomic analysis of TCs and MCs using an Ultimate 3000 RSLC nanoHPLC system connected to a QExactive Plus mass spectrometer. Results. The study of the proteomic profiles of M. hominis colonies allowed us to reconstruct their energy metabolism pathways. In addition to the already known pentose phosphate and arginine deamination pathways, M. hominis can utilise ribose phosphate and deoxyribose phosphate formed by nucleoside catabolism as energy sources. Comparative proteomic HPLC–MS analysis revealed that the proteomic profiles of TCs and MCs were different. We assume that MC cells preferably utilised deoxyribonucleosides, particularly thymidine, as an energy source rather than arginine or ribonucleosides. Utilisation of deoxyribonucleosides is less efficient as compared with that of ribonucleosides and arginine in terms of energy production. Thymidine phosphorylase DeoA is one of the key enzymes of deoxyribonucleosides utilisation. We obtained a DeoA overexpressing mutant that exhibited a phenotype similar to that of MCs, which confirmed our hypothesis. Conclusion. In addition to the two known pathways for energy production (arginine deamination and the pentose phosphate pathway) M. hominis can use deoxyribonucleosides and ribonucleosides. MC cells demonstrate a reorganisation of energy metabolism: unlike TC cells, they preferably utilise deoxyribonucleosides, particularly thymidine, as an energy source rather than arginine or ribonucleosides. Thus MC cells enter a state of energy starvation, which helps them to survive under stress, and in particular, to be resistant to antibiotics.

Published

2022

8. Proteome of HU-Lacking E. coli Studied by Means of 2D Gel Electrophoresis

Author

V. E. Anisimova, A. L. Drobyshev, O. V. Pobeguts, Gleb Y. Fisunov, Yu. K. Agapova, D. E. Kamashev, Daria Matyushkina, Tatiana V. Rakitina, Daria V. Evsyutina, Ivan Butenko, and Anna Vanyushkina

Subjects

0301 basic medicine, Regulation of gene expression, 010405 organic chemistry, Microarray analysis techniques, Organic Chemistry, HU Protein, Bacterial nucleoid, 01 natural sciences, Biochemistry, Molecular biology, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Regulon, chemistry, Gene expression, Proteome, DNA

Abstract

Histone-like protein HU is a dimeric nucleoid-associated protein (NAP). HU is the most conserved NAP. It binds nonspecifically to duplex DNA with a preference for targeting nicked and bent DNA. HU limits the architecture of the bacterial nucleoid and its deletion is lethal for Bacillus subtilis and Mycoplasma genitalium which do not contain other NAPs. E. coli lacking HU is viable but has numerous growth defects. The effects of the HU protein on gene expression is known from microarray analysis and HU regulons were identified. In HU-deficient E. coli, absence of this DNA architectural protein causes a disorder in gene regulation; on the other hand, E. coli growth under standard conditions is almost unaltered in the absence of HU. To understand how the bacterium confronts the chromosomal disorder, we performed proteome analysis to compare protein abundances in cells containing the HU protein or not. Comparison of the proteomic profile of wild-type and HU-deficient E. coli shows how the altered gene expression influences the protein content. We show that proteome profile changes are very similar to the gene expression profile changes in HU-deficient E. coli. Several exceptions show that proteome studies are very important.

Published

2019

9. Propionate Induces Virulent Properties of Crohn’s Disease-Associated Escherichia coli

Author

Daria Matyushkina, A. I. Zubov, V. G. Ladygina, Daria V. Evsyutina, Artem V. Eremeev, Daria V. Rakitina, Gleb Y. Fisunov, Peter L. Scherbakov, and Olga Pobeguts

Subjects

Microbiology (medical), Crohn’s disease, propionic acid, lcsh:QR1-502, Virulence, medicine.disease_cause, Microbiology, lcsh:Microbiology, Pathogenesis, 03 medical and health sciences, medicine, Macrophage, Escherichia coli, Transcription factor, 030304 developmental biology, Original Research, chemistry.chemical_classification, 0303 health sciences, Gastrointestinal tract, 030306 microbiology, Chemistry, Crohn’s disease-associated adherent-invasive Escherichia coli, Phenotype, macrophages, Propionate, bacteria, 2D electrophoresis

Abstract

Crohn's disease (CD) is a severe chronic immune-mediated granulomatous inflammatory disease of the gastrointestinal tract. The mechanisms of CD pathogenesis remain obscure. Metagenomic analysis of samples from CD patients revealed that several of them have the elevated level of Escherichia coli with adhesive-invasive phenotype (AIEC). Previously, we isolated an E. coli strain CD isolate ZvL2 from a patient with CD, which features AIEC phenotype. Here, we demonstrate that prolonged growth on propionate containing medium stimulates virulent properties of CD isolate ZvL2, while prolonged growth on glucose reduces these properties to levels indistinguishable from laboratory strain K-12 MG1655. Propionate presence also boosts the ability of CD isolate ZvL2 to penetrate and colonize macrophages. The effect of propionate is reversible, re-passaging of CD isolate on M9 medium supplemented with glucose leads to the loss of its virulent properties. Proteome analysis of CD isolate ZvL2 growth in medium supplemented with propionate or glucose revealed that propionate induces expression porins OmpA and OmpW, transcription factors PhoP and OmpR, and universal stress protein UspE, which were previously found to be important for macrophage colonization by enteropathogenic bacteria.

Published

2020

10. Data on proteome of

Author

V. G. Ladygina, Tatiana A. Semashko, A. I. Zubov, O. V. Pobeguts, Rustam H. Ziganshin, Irina V. Rakovskaya, Daria V. Evsyutina, and Sergey I. Kovalchuk

Subjects

Proteome, Mycoplasma hominis, Arginine, lcsh:Computer applications to medicine. Medical informatics, Cultivation conditions, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Mutase, Biochemistry, Genetics and Molecular Biology, Thymidine phosphorylase, lcsh:Science (General), 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, biology.organism_classification, Metabolic pathway, chemistry, Biochemistry, Carbon source, lcsh:R858-859.7, Energy source, Thymidine, 030217 neurology & neurosurgery, Bacteria, lcsh:Q1-390

Abstract

Mycoplasma hominis is an opportunistic bacterium that can cause acute and chronic infections of the urogenital tract. This bacterium, like all other Mycoplasma species, is characterized by the reduced genome size, and, consequently, reduction of the main metabolic pathways. M. hominis cells cannot effectively use glucose as a carbon and energy source. Therefore, the main pathway of energy metabolism is the arginine dihydrolase pathway. However, several bacteria can use nucleosides as the sole energy source. Biochemical studies using Salmonella typhimurium have shown that three enzymes (thymidine phosphorylase, phosphopentose mutase and deoxyribose-phosphate aldolase) are involved in the thymidine catabolic pathway. All these enzymes are present in M. hominis. For understanding changes in the energy metabolism of M. hominis we performed shotgun proteome analysis of M. hominis cells in liquid medium with arginine or thymidine as a carbon source. LC-MS analysis was performed with an Ultimate 3000 Nano LC System (Thermo Fisher Scientific) coupled to a Q Exactive HF benchtop Orbitrap mass spectrometer (Thermo Fisher Scientific) via a nanoelectrospray source (Thermo Fisher Scientific). Data are available via ProteomeXchange with identifier PXD018714 (https://www.ebi.ac.uk/pride/archive/projects/PXD018714).

Published

2020

11. ANTIBIOTIC RESISTANCE AND PROTEOMIC ANALYSIS OF MICROCOLONIES MYCOPLASMA HOMINIS

Author

G.Yu. Fisunov, V. G. Ladygina, G.A. Levina, O.I. Barhatova, A. I. Zubov, O. V. Pobeguts, Rustam Ziganshin, Sergey I. Kovalchuk, Daria V. Evsyutina, I V Rakovskaya, and N.F. Gamaleya Nrcem

Subjects

Antibiotic resistance, Mycoplasma hominis, Biology, biology.organism_classification, Microbiology

Published

2020

12. Binding site of MraZ transcription factor in Mollicutes

Author

Tatiana A. Semashko, Gleb Y. Fisunov, Daria V. Evsyutina, Valentin A. Manuvera, Andrey V. Letarov, Aleksandr A. Arzamasov, and Vadim M. Govorun

Subjects

0301 basic medicine, Mycoplasma gallisepticum, Transcription, Genetic, Operon, 030106 microbiology, Mollicutes, Response Elements, Biochemistry, 03 medical and health sciences, Mycoplasma, Bacterial Proteins, Transcription (biology), Direct repeat, Histone octamer, Binding site, Gene, Genetics, biology, General Medicine, biology.organism_classification, Molecular biology, 030104 developmental biology, Transcription factor, Transcription, Transcription Factors

Abstract

Mollicutes (mycoplasmas) feature a significant loss of known regulators of gene expression. Here, we identified the recognition site of the MraZ-family regulator of Mycoplasma gallisepticum, which is conserved in many species of different clades within class Mollicutes. The MraZ binding site is AAAGTG[T/G], in the promoter of mraZ gene it forms a series of direct repeats with a structure (AAAGTG[T/G]N3)k, where k = 3 most frequently. MraZ binds to a single repeat as an octamer complex. MraZ can also bind a single binding site or a series of repeats with different spacer lengths (2–4 nt); thus, it may play a role in the regulation of multiple operons in Mollicutes. In M. gallisepticum, MraZ acts as a transcriptional activator. The overexpression of MraZ leads to moderate filamentation of cells and the formation of aggregates, likely as a result of incomplete cytokinesis.

Published

2016

13. Reconstruction of transcription control networks in Mollicutes by high-throughput identification of promoters

Author

Daria V. Evsyutina, Tatiana A. Semashko, Irina A. Garanina, Gleb Y. Fisunov, Anastasia S. Nikitina, and Vadim M. Govorun

Subjects

0301 basic medicine, Microbiology (medical), Mycoplasma gallisepticum, Spiroplasma, 030106 microbiology, Mollicutes, lcsh:QR1-502, Microbiology, lcsh:Microbiology, 03 medical and health sciences, Mycoplasma, transcription factors, Transcriptional regulation, medicine, Transcriptomics, Transcription factor, Original Research, Genetics, biology, Promoter, biology.organism_classification, medicine.disease, Acholeplasma, Transcriptional noise

Abstract

Bacteria of the class Mollicutes have significantly reduced genomes and gene expression control systems. They are also efficient pathogens that can colonize a broad range of hosts including plants and animals. Despite their simplicity, Mollicutes demonstrate complex transcriptional responses to various conditions, which contradicts their reduction in gene expression regulation mechanisms. We analyzed the conservation and distribution of transcription regulators across the 50 Mollicutes species. The majority of the transcription factors regulate transport and metabolism, and there are four transcription factors that demonstrate significant conservation across the analyzed bacteria. These factors include repressors of chaperone HrcA, cell cycle regulator MraZ and two regulators with unclear function from the WhiA and YebC/PmpR families. We then used three representative species of the major clades of Mollicutes (Acholeplasma laidlawii, Spiroplasma melliferum and Mycoplasma gallisepticum) to perform promoters mapping and activity quantitation. We revealed that Mollicutes evolved towards a promoter architecture simplification that correlates with a diminishing role of transcription regulation and an increase in transcriptional noise. Using the identified operons structure and a comparative genomics approach, we reconstructed the transcription control networks for these three species. The organization of the networks reflects the adaptation of bacteria to specific conditions and hosts.

Published

2016

14. Phase Transition of the Bacterium upon Invasion of a Host Cell as a Mechanism of Adaptation: a Mycoplasma gallisepticum Model

Author

Maria A. Lagarkova, Tatiana A. Semashko, Daria Matyushkina, V. G. Ladygina, Olga Pobeguts, A. N. Bogomazova, Ivan Butenko, Vladislav V. Babenko, Anna Vanyushkina, Vadim M. Govorun, Olga Bukato, Maria T. Vakhitova, Irina A. Garanina, Daria V. Evsyutina, Gleb Y. Fisunov, and Nicolay Anikanov

Subjects

0301 basic medicine, Mycoplasma gallisepticum, Proteome, 030106 microbiology, Cell, Adaptation, Biological, Biology, medicine.disease_cause, Article, Bacterial cell structure, Cell Line, Microbiology, Mice, 03 medical and health sciences, medicine, Animals, Humans, Serial Passage, Pathogen, Multidisciplinary, Gene Expression Profiling, Gene Expression Regulation, Bacterial, Mycoplasma, biology.organism_classification, Adaptation, Physiological, Endocytosis, medicine.anatomical_structure, Cell culture, Metabolome, Chickens, Intracellular

Abstract

What strategies do bacteria employ for adaptation to their hosts and are these strategies different for varied hosts? To date, many studies on the interaction of the bacterium and its host have been published. However, global changes in the bacterial cell in the process of invasion and persistence, remain poorly understood. In this study, we demonstrated phase transition of the avian pathogen Mycoplasma gallisepticum upon invasion of the various types of eukaryotic cells (human, chicken, and mouse) which was stable during several passages after isolation of intracellular clones and recultivation in a culture medium. It was shown that this phase transition is manifested in changes at the proteomic, genomic and metabolomic levels. Eukaryotic cells induced similar proteome reorganization of M. gallisepticum during infection, despite different origins of the host cell lines. Proteomic changes affected a broad range of processes including metabolism, translation and oxidative stress response. We determined that the activation of glycerol utilization, overproduction of hydrogen peroxide and the upregulation of the SpxA regulatory protein occurred during intracellular infection. We propose SpxA as an important regulator for the adaptation of M. gallisepticum to an intracellular environment.

Published

2016

15. Ribosome profiling reveals an adaptation strategy of reduced bacterium to acute stress

Author

Daria V. Evsyutina, Ivan Butenko, Irina A. Garanina, Anastasia S. Nikitina, Ilya Altukhov, Gleb Y. Fisunov, Vadim M. Govorun, and Aleksandr A. Arzamasov

Subjects

0301 basic medicine, Hot Temperature, Proteome, Systems biology, HU Protein, ved/biology.organism_classification_rank.species, Mollicutes, Mycoplasma gallisepticum, Biology, Ribosome profiling, Stress, Ribosome, Biochemistry, 03 medical and health sciences, Mycoplasma, Bacterial Proteins, Transcription (biology), Stress, Physiological, Tandem Mass Spectrometry, RNA, Messenger, ORFS, Model organism, Chromatography, High Pressure Liquid, Genetics, Base Sequence, ved/biology, Gene Expression Profiling, General Medicine, Gene Expression Regulation, Bacterial, Adaptation, Physiological, 030104 developmental biology, Protein Biosynthesis, Ribosomes, Heat-Shock Response

Abstract

Bacteria of class Mollicutes (mycoplasmas) feature significant genome reduction which makes them good model organisms for systems biology studies. Previously we demonstrated, that drastic transcriptional response of mycoplasmas to stress results in a very limited response on the level of protein. In this study we used heat stress model of M. gallisepticum and ribosome profiling to elucidate the process of genetic information transfer under stress. We found that under heat stress ribosomes demonstrate selectivity towards mRNA binding. We identified that heat stress response may be divided into two groups on the basis of absolute transcript abundance and fold-change in the translatome. One represents a noise-like response and another is likely an adaptive one. The latter include ClpB chaperone, cell division cluster, homologs of immunoblocking proteins and short ORFs with unknown function. We found that previously identified read-through of terminators contributes to the upregulation of transcripts in the translatome as well. In addition we identified that ribosomes of M. gallisepticum undergo reorganization under the heat stress. The most notable event is decrease of the amount of associated HU protein. In conclusion, only changes of few adaptive transcripts significantly impact translatome, while widespread noise-like transcription plays insignificant role in translation during stress.

Published

2016

16. Binding site of restriction-modification system controller protein in Mollicutes

Author

Vadim M. Govorun, Daria V. Evsyutina, Valentin A. Manuvera, and Gleb Y. Fisunov

Subjects

0301 basic medicine, Mycoplasma gallisepticum, Microbiology (medical), Transcription, Genetic, Operon, Mollicutes, Microbiology, 03 medical and health sciences, Mycoplasma, Bacterial Proteins, RNA, Transfer, Direct repeat, DNA Restriction-Modification Enzymes, Binding site, Promoter Regions, Genetic, Genetics, Tenericutes, Binding Sites, 030102 biochemistry & molecular biology, biology, Chromosome Mapping, Promoter, Endopeptidase Clp, Gene Expression Regulation, Bacterial, biology.organism_classification, Restriction-modification, 030104 developmental biology, Genes, Bacterial, Restriction modification system, Transcription factor, Protein Processing, Post-Translational, Research Article, Regulation, Protein Binding, Transcription Factors

Abstract

Background Bacteria of the class Mollicutes underwent extreme reduction of genomes and gene expression control systems. Only a few regulators are known to date. In this work, we describe a novel group of transcriptional regulators that are distributed within different Mollicutes and control the expression of restriction-modification systems (RM-systems). Results We performed cross-species search of putative regulators of RM-systems (C-proteins) and respective binding sites in Mollicutes. We identified a set of novel putative C-protein binding motifs distributed within Mollicutes. We studied the most frequent motif and respective C-protein on the model of Mycoplasma gallisepticum S6. We confirmed our prediction and identified key nucleotides important for C-protein binding. Further we identified novel target promoters of C-protein in M. gallisepticum. Conclusions We found that C-protein of M. gallisepticum binds predicted conserved direct repeats of the (GTGTTAN5)2 motif. Apart from its own operon promoter, HsdC can bind to the promoters of the clpB chaperone gene and a tRNA cluster. Electronic supplementary material The online version of this article (doi:10.1186/s12866-017-0935-4) contains supplementary material, which is available to authorized users.

17. Reconstruction of transcription control networks in Mollicutes by high-throughput identification of promoters

Author

Gleb Y Fisunov, Irina A Garanina, Daria V Evsyutina, Tatiana A Semashko, Anastasia S Nikitina, and Vadim Markovich Govorun

Subjects

Acholeplasma, Mycoplasma, Spiroplasma, Promoter, Transcriptomics, Mollicutes, Microbiology, QR1-502

Abstract

Bacteria of the class Mollicutes have significantly reduced genomes and gene expression control systems. They are also efficient pathogens that can colonize a broad range of hosts including plants and animals. Despite their simplicity, Mollicutes demonstrate complex transcriptional responses to various conditions, which contradicts their reduction in gene expression regulation mechanisms. We analyzed the conservation and distribution of transcription regulators across the 50 Mollicutes species. The majority of the transcription factors regulate transport and metabolism, and there are four transcription factors that demonstrate significant conservation across the analyzed bacteria. These factors include repressors of chaperone HrcA, cell cycle regulator MraZ and two regulators with unclear function from the WhiA and YebC/PmpR families. We then used three representative species of the major clades of Mollicutes (Acholeplasma laidlawii, Spiroplasma melliferum and Mycoplasma gallisepticum) to perform promoters mapping and activity quantitation. We revealed that Mollicutes evolved towards a promoter architecture simplification that correlates with a diminishing role of transcription regulation and an increase in transcriptional noise. Using the identified operons structure and a comparative genomics approach, we reconstructed the transcription control networks for these three species. The organization of the networks reflects the adaptation of bacteria to specific conditions and hosts.

Published

2016