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1. Enterobacteriaceae Growth Promotion by Intestinal Acylcarnitines, a Biomarker of Dysbiosis in Inflammatory Bowel DiseaseSummary

Author

Johanna M.S. Lemons, Maire Conrad, Ceylan Tanes, Jie Chen, Elliot S. Friedman, Manuela Roggiani, Dylan Curry, Lillian Chau, Aaron L. Hecht, Lisa Harling, Jennifer Vales, Kelly E. Kachelries, Robert N. Baldassano, Mark Goulian, Kyle Bittinger, Stephen R. Master, LinShu Liu, and Gary D. Wu

Subjects
Microbiota, IBD, Metabolism, Carnitine, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background & Aims: Altered plasma acylcarnitine levels are well-known biomarkers for a variety of mitochondrial fatty acid oxidation disorders and can be used as an alternative energy source for the intestinal epithelium when short-chain fatty acids are low. These membrane-permeable fatty acid intermediates are excreted into the gut lumen via bile and are increased in the feces of patients with inflammatory bowel disease (IBD). Methods: Herein, based on studies in human subjects, animal models, and bacterial cultures, we show a strong positive correlation between fecal carnitine and acylcarnitines and the abundance of Enterobacteriaceae in IBD where they can be consumed by bacteria both in vitro and in vivo. Results: Carnitine metabolism promotes the growth of Escherichia coli via anaerobic respiration dependent on the cai operon, and acetylcarnitine dietary supplementation increases fecal carnitine levels with enhanced intestinal colonization of the enteric pathogen Citrobacter rodentium. Conclusions: In total, these results indicate that the increased luminal concentrations of carnitine and acylcarnitines in patients with IBD may promote the expansion of pathobionts belonging to the Enterobacteriaceae family, thereby contributing to disease pathogenesis.

Published
2024
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2. Phage integration alters the respiratory strategy of its host

Author

Jeffrey N Carey, Erin L Mettert, Daniel R Fishman-Engel, Manuela Roggiani, Patricia J Kiley, and Mark Goulian

Subjects
bacteriophage, trimethylamine N-oxide, two-component signaling, bet hedging, Medicine, Science, Biology (General), QH301-705.5
Abstract

Temperate bacteriophages are viruses that can incorporate their genomes into their bacterial hosts, existing there as prophages that refrain from killing the host cell until induced. Prophages are largely quiescent, but they can alter host phenotype through factors encoded in their genomes (often virulence factors) or by disrupting host genes as a result of integration. Here we describe another mechanism by which a prophage can modulate host phenotype. We show that a temperate phage that integrates in Escherichia coli reprograms host regulation of an anaerobic respiratory system, thereby inhibiting a bet hedging strategy. The phage exerts this effect by upregulating a host-encoded signal transduction protein through transcription initiated from a phage-encoded promoter. We further show that this phenomenon occurs not only in a laboratory strain of E. coli, but also in a natural isolate that contains a prophage at this site.

Published
2019
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3. Antimicrobial peptides trigger a division block in Escherichia coli through stimulation of a signalling system

Author

Srujana S. Yadavalli, Jeffrey N. Carey, Rachel S. Leibman, Annie I. Chen, Andrew M. Stern, Manuela Roggiani, Andrew M. Lippa, and Mark Goulian

Subjects
Science
Abstract

The PhoQ/PhoP system regulates antimicrobial peptide defense in bacteria. Here the authors show that at sublethal concentrations of antimicrobial peptides, PhoPQ induces QueE, that then localizes to the divisome and blocks cell division independently of its function in queuosine biosynthesis.

Published
2016
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4. Deciphering the Role of Colicins during Colonization of the Mammalian Gut by Commensal E. coli

Author

Amanda N. Samuels, Manuela Roggiani, Kathryn A. Smith, Jun Zhu, Mark Goulian, and Rahul M. Kohli

Subjects
colonization, colicin, commensal E. coli, DNA damage response, Biology (General), QH301-705.5
Abstract

Colicins are specific and potent toxins produced by Enterobacteriaceae that result in the rapid elimination of sensitive cells. Colicin production is commonly found throughout microbial populations, suggesting its potential importance for bacterial survival in complex microbial environments. Nonetheless, as colicin biology has been predominately studied using synthetic models, it remains unclear how colicin production contributes to survival and fitness of a colicin-producing commensal strain in a natural environment. To address this gap, we took advantage of MP1, an E. coli strain that harbors a colicinogenic plasmid and is a natural colonizer of the murine gut. Using this model, we validated that MP1 is competent for colicin production and then directly interrogated the importance of colicin production and immunity for MP1 survival in the murine gut. We showed that colicin production is dispensable for sustained colonization in the unperturbed gut. A strain lacking colicin production or immunity shows minimal fitness defects and can resist displacement by colicin producers. This report extends our understanding of the role that colicin production may play for E. coli during gut colonization and suggests that colicin production is not essential for a commensal to persist in its physiologic niche in the absence of exogenous challenges.

Published
2020
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5. Natural variation of a sensor kinase controlling a conserved stress response pathway in Escherichia coli.

Author

Manuela Roggiani, Srujana S Yadavalli, and Mark Goulian

Subjects
Genetics, QH426-470
Abstract

Previous studies have shown that exponentially growing Escherichia coli can detect mild acidity (~pH 5.5) and, in response, synthesize enzymes that protect against severe acid shock. This adaptation is controlled by the EvgS/EvgA phosphorelay, a signal transduction system present in virtually every E. coli isolate whose genome has been sequenced. Here we show that, despite this high level of conservation, the EvgS/EvgA system displays a surprising natural variation in pH-sensing capacity, with some strains entirely non-responsive to low pH stimulus. In most cases that we have tested, however, activation of the EvgA regulon still confers acid resistance. From analyzing selected E. coli isolates, we find that the natural variation results from polymorphisms in the sensor kinase EvgS. We further show that this variation affects the pH response of a second kinase, PhoQ, which senses pH differently from the closely related PhoQ in Salmonella enterica. The within-species diversification described here suggests EvgS likely responds to additional input signals that may be correlated with acid stress. In addition, this work highlights the fact that even for highly conserved sensor kinases, the activities identified from a subset of isolates may not necessarily generalize to other members of the same bacterial species.

Published
2017
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6. Systematically Altering Bacterial SOS Activity under Stress Reveals Therapeutic Strategies for Potentiating Antibiotics

Author

Charlie Y. Mo, Sara A. Manning, Manuela Roggiani, Matthew J. Culyba, Amanda N. Samuels, Paul D. Sniegowski, Mark Goulian, and Rahul M. Kohli

Subjects
DNA damage, LexA, RecA, SOS pathway, adjuvant therapy, antibiotic resistance, Microbiology, QR1-502
Abstract

ABSTRACT The bacterial SOS response is a DNA damage repair network that is strongly implicated in both survival and acquired drug resistance under antimicrobial stress. The two SOS regulators, LexA and RecA, have therefore emerged as potential targets for adjuvant therapies aimed at combating resistance, although many open questions remain. For example, it is not well understood whether SOS hyperactivation is a viable therapeutic approach or whether LexA or RecA is a better target. Furthermore, it is important to determine which antimicrobials could serve as the best treatment partners with SOS-targeting adjuvants. Here we derived Escherichia coli strains that have mutations in either lexA or recA genes in order to cover the full spectrum of possible SOS activity levels. We then systematically analyzed a wide range of antimicrobials by comparing the mean inhibitory concentrations (MICs) and induced mutation rates for each drug-strain combination. We first show that significant changes in MICs are largely confined to DNA-damaging antibiotics, with strains containing a constitutively repressed SOS response impacted to a greater extent than hyperactivated strains. Second, antibiotic-induced mutation rates were suppressed when SOS activity was reduced, and this trend was observed across a wider spectrum of antibiotics. Finally, perturbing either LexA or RecA proved to be equally viable strategies for targeting the SOS response. Our work provides support for multiple adjuvant strategies, while also suggesting that the combination of an SOS inhibitor with a DNA-damaging antibiotic could offer the best potential for lowering MICs and decreasing acquired drug resistance. IMPORTANCE Our antibiotic arsenal is becoming depleted, in part, because bacteria have the ability to rapidly adapt and acquire resistance to our best agents. The SOS pathway, a widely conserved DNA damage stress response in bacteria, is activated by many antibiotics and has been shown to play central role in promoting survival and the evolution of resistance under antibiotic stress. As a result, targeting the SOS response has been proposed as an adjuvant strategy to revitalize our current antibiotic arsenal. However, the optimal molecular targets and partner antibiotics for such an approach remain unclear. In this study, focusing on the two key regulators of the SOS response, LexA and RecA, we provide the first comprehensive assessment of how to target the SOS response in order to increase bacterial susceptibility and reduce mutagenesis under antibiotic treatment.

Published
2016
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7. A commensal-encoded genotoxin drives restriction of

Author

Jiandong, Chen, Hyuntae, Byun, Rui, Liu, I-Ji, Jung, Qinqin, Pu, Clara Y, Zhu, Ethan, Tanchoco, Salma, Alavi, Patrick H, Degnan, Amy T, Ma, Manuela, Roggiani, Joris, Beld, Mark, Goulian, Ansel, Hsiao, and Jun, Zhu

Subjects
Prognosis, Gastrointestinal Microbiome, Disease Models, Animal, Mice, Cholera, Polyketides, Antibiosis, Host-Pathogen Interactions, Escherichia coli, Animals, Humans, Microbial Interactions, Peptides, Reactive Oxygen Species, Vibrio cholerae, DNA Damage, Mutagens
Abstract

SignificanceIn a polymicrobial battlefield where different species compete for nutrients and colonization niches, antimicrobial compounds are the sword and shield of commensal microbes in competition with invading pathogens and each other. The identification of an

Published
2022

8. Deciphering the Role of Colicins during Colonization of the Mammalian Gut by Commensal E. coli

Author

Mark Goulian, Manuela Roggiani, Kathryn A. Smith, Amanda N. Samuels, Rahul M. Kohli, and Jun Zhu

Subjects
Microbiology (medical), inorganic chemicals, Biology, DNA damage response, Microbiology, Article, 03 medical and health sciences, Coli strain, Plasmid, Immunity, Virology, Colonization, lcsh:QH301-705.5, 030304 developmental biology, 0303 health sciences, Gut colonization, 030306 microbiology, technology, industry, and agriculture, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, colonization, Enterobacteriaceae, lcsh:Biology (General), commensal E. coli, Colicin, bacteria, lipids (amino acids, peptides, and proteins), colicin
Abstract

Colicins are specific and potent toxins produced by Enterobacteriaceae that result in the rapid elimination of sensitive cells. Colicin production is commonly found throughout microbial populations, suggesting its potential importance for bacterial survival in complex microbial environments. Nonetheless, as colicin biology has been predominately studied using synthetic models, it remains unclear how colicin production contributes to survival and fitness of a colicin-producing commensal strain in a natural environment. To address this gap, we took advantage of MP1, an E. coli strain that harbors a colicinogenic plasmid and is a natural colonizer of the murine gut. Using this model, we validated that MP1 is competent for colicin production and then directly interrogated the importance of colicin production and immunity for MP1 survival in the murine gut. We showed that colicin production is dispensable for sustained colonization in the unperturbed gut. A strain lacking colicin production or immunity shows minimal fitness defects and can resist displacement by colicin producers. This report extends our understanding of the role that colicin production may play for E. coli during gut colonization and suggests that colicin production is not essential for a commensal to persist in its physiologic niche in the absence of exogenous challenges.

Published
2020

9. Phage integration alters the respiratory strategy of its host

Author

Daniel R Fishman-Engel, Jeffrey N. Carey, Erin L. Mettert, Mark Goulian, Patricia J. Kiley, and Manuela Roggiani

Subjects
0301 basic medicine, QH301-705.5, viruses, Prophages, Virus Integration, Science, 030106 microbiology, Biology, medicine.disease_cause, Coliphages, General Biochemistry, Genetics and Molecular Biology, Bacterial cell structure, Microbiology, Bacteriophage, 03 medical and health sciences, chemistry.chemical_compound, bacteriophage, Gene expression, medicine, Escherichia coli, Anaerobiosis, Biology (General), Gene, bet hedging, Microbiology and Infectious Disease, General Immunology and Microbiology, trimethylamine N-oxide, Host (biology), General Neuroscience, fungi, E. coli, General Medicine, Gene Expression Regulation, Bacterial, biology.organism_classification, Chromosomes and Gene Expression, 030104 developmental biology, chemistry, Medicine, two-component signaling, Energy Metabolism, DNA, Bacteria, Signal Transduction, Research Article
Abstract

Temperate bacteriophages are viruses that can incorporate their genomes into their bacterial hosts, existing there as prophages that refrain from killing the host cell until induced. Prophages are largely quiescent, but they can alter host phenotype through factors encoded in their genomes (often virulence factors) or by disrupting host genes as a result of integration. Here we describe another mechanism by which a prophage can modulate host phenotype. We show that a temperate phage that integrates in Escherichia coli reprograms host regulation of an anaerobic respiratory system, thereby inhibiting a bet hedging strategy. The phage exerts this effect by upregulating a host-encoded signal transduction protein through transcription initiated from a phage-encoded promoter. We further show that this phenomenon occurs not only in a laboratory strain of E. coli, but also in a natural isolate that contains a prophage at this site., eLife digest Animals and plants can all fall prey to viruses – and so can bacteria. The viruses that infect bacteria are called bacteriophages (or phages for short), and they are found everywhere bacteria live and probably outnumber bacteria by at least ten to one. While some phages quickly kill every bacterial cell they infect, others enter a dormant state by inserting their DNA into the DNA of their host cell. Here they lie in wait for a signal that reactivates them, triggering the production of more phages and the death of the host cell. While the phage lies dormant its DNA may harm the host by interfering with nearby bacterial genes, or it may actually provide new genes that benefit the host. In most cases the effects of dormant phages are unknown. A bacterium known as Escherichia coli is commonly found in the intestines of humans and other mammals. It can use a nutrient called trimethylamine oxide (TMAO) to help it survive rapid decreases in oxygen levels that can occur in its environment. When a phage called HK022 infects E. coli, the phage enters a dormant state by inserting its DNA between two genes that are critical for E. coli to use TMAO. However, it is not clear what effect, if any, HK022 has on E. coli’s behavior. To address this question, Carey et al. used genetic approaches to study E. coli cells carrying dormant HK022 phages. The experiments showed that the bacteria lost the ability to use TMAO to survive rapid decreases in oxygen because the dormant phages switched on one of the neighboring E. coli genes. Unexpectedly, the phage achieved this by neatly replacing the gene’s own promoter – the stretch of DNA that contains information about when the gene should be switched on, and how strongly – with a substitute promoter carried in the phage’s DNA. This substitute promoter is stronger than the normal version – meaning that the gene is more active than it should be. Phages are key players in every natural population of microbes and are therefore entwined in the health of humans and the environment. The findings of Carey et al. show a new mechanism through which phages modify their hosts. In the future it may be possible to develop this mechanism into a tool to manipulate bacteria in complex environments like infection sites, for example by introducing phages that block the mechanisms that allow bacteria to tolerate antibiotics.

Published
2019

11. The SOS Response Mediates Sustained Colonization of the Mammalian Gut

Author

Jun Zhu, Mark Goulian, Manuela Roggiani, Rahul M. Kohli, and Amanda N. Samuels

Subjects
DNA repair, DNA damage, Immunology, Context (language use), Genotoxic Stress, Biology, medicine.disease_cause, Microbiology, Mice, Escherichia coli, medicine, Animals, Colonization, Microbiome, SOS response, SOS Response, Genetics, Gene Expression Regulation, Bacterial, Host-Associated Microbial Communities, Gastrointestinal Tract, Mice, Inbred C57BL, Disease Models, Animal, Infectious Diseases, bacteria, Parasitology, DNA Damage
Abstract

Bacteria have a remarkable ability to survive, persist, and ultimately adapt to environmental challenges. A ubiquitous environmental hazard is DNA damage, and most bacteria have evolved a network of genes to combat genotoxic stress. This network is known as the SOS response and aids in bacterial survival by regulating genes involved in DNA repair and damage tolerance. Recently, the SOS response has been shown to play an important role in bacterial pathogenesis, and yet the role of the SOS response in nonpathogenic organisms and in physiological settings remains underexplored. Using a commensal Escherichia coli strain, MP1, we showed that the SOS response plays a vital role during colonization of the murine gut. In an unperturbed environment, the SOS-off mutant is impaired for stable colonization relative to a wild-type strain, suggesting the presence of genotoxic stress in the mouse gut. We evaluated the possible origins of genotoxic stress in the mouse gut by examining factors associated with the host versus the competing commensal organisms. In a dextran sulfate sodium (DSS) colitis model, the SOS-off colonization defect persisted but was not exacerbated. In contrast, in a germ-free model, the SOS-off mutant colonized with efficiency equal to that seen with the wild-type strain, suggesting that competing commensal organisms might be a significant source of genotoxic stress. This report extends our understanding of the importance of a functional SOS response for bacterial fitness in the context of a complex physiological environment and highlights the SOS response as a possible mechanism that contributes to ongoing genomic changes, including potential antibiotic resistance, in the microbiome of healthy hosts.

Published
2019

13. The phosphohistidine phosphatase SixA dephosphorylates the phosphocarrier NPr

Author

Jun Zhu, Manuela Roggiani, Hui Shi, Mark Goulian, and Jane E. Schulte

Subjects
0301 basic medicine, phosphoryl transfer, (His)6 or (His)8, polyhistidine, π-pHis, π-phosphohistidine, phosphoramidate hydrolase, Phosphatase, τ-pHis, τ-phosphohistidine, NPr-P, phosphorylated NPr, lac operon, Phosphocarrier protein, ECL, enhanced chemiluminescence, Biochemistry, TEV, tobacco etch virus, Dephosphorylation, 03 medical and health sciences, CFU, colony forming units, Bacterial Proteins, Ptrc, trc promoter, Escherichia coli, TBST, Tris-buffered saline and Tween solution, phosphotransferase system, IPTG, isopropyl-β-D-thiogalactopyranoside, Histidine, Protein phosphorylation, Phosphorylation, B-PER, bacterial protein extraction reagent, Molecular Biology, 030102 biochemistry & molecular biology, biology, Chemistry, FRT, FLP recombination target, PEP, phosphoenolpyruvate, Cell Biology, PEP group translocation, Phosphoric Monoester Hydrolases, protein phosphorylation, SixA-P, phosphorylated SixA, 030104 developmental biology, cross talk, bacterial protein phosphatase, biology.protein, Research Article, Signal Transduction
Abstract

Histidine phosphorylation is a posttranslational modification that alters protein function and also serves as an intermediate of phosphoryl transfer. Although phosphohistidine is relatively unstable, enzymatic dephosphorylation of this residue is apparently needed in some contexts, since both prokaryotic and eukaryotic phosphohistidine phosphatases have been reported. Here we identify the mechanism by which a bacterial phosphohistidine phosphatase dephosphorylates the nitrogen-related phosphotransferase system, a broadly conserved bacterial pathway that controls diverse metabolic processes. We show that the phosphatase SixA dephosphorylates the phosphocarrier protein NPr and that the reaction proceeds through phosphoryl transfer from a histidine on NPr to a histidine on SixA. In addition, we show that Escherichia coli lacking SixA are outcompeted by wild-type E. coli in the context of commensal colonization of the mouse intestine. Notably, this colonization defect requires NPr and is distinct from a previously identified in vitro growth defect associated with dysregulation of the nitrogen-related phosphotransferase system. The widespread conservation of SixA, and its coincidence with the phosphotransferase system studied here, suggests that this dephosphorylation mechanism may be conserved in other bacteria.

Published
2021

14. Antimicrobial peptides trigger a division block in Escherichia coli through stimulation of a signalling system

Author

Manuela Roggiani, Andrew M. Stern, Srujana S. Yadavalli, Jeffrey N. Carey, Annie I. Chen, Mark Goulian, Rachel S. Leibman, and Andrew M. Lippa

Subjects
0301 basic medicine, Cytoplasm, TRNA modification, Transcription, Genetic, Cell division, Science, Antimicrobial peptides, Regulator, General Physics and Astronomy, medicine.disease_cause, Models, Biological, Article, General Biochemistry, Genetics and Molecular Biology, Microbiology, 03 medical and health sciences, Chromosome Segregation, Escherichia coli, Nucleoside Q, medicine, Regulation of gene expression, Multidisciplinary, biology, Escherichia coli Proteins, Gene Expression Regulation, Bacterial, General Chemistry, Antimicrobial, biology.organism_classification, Biosynthetic Pathways, 3. Good health, 030104 developmental biology, Cell Division, Gene Deletion, Bacteria, Antimicrobial Cationic Peptides, Signal Transduction
Abstract

Antimicrobial peptides are an important component of the molecular arsenal employed by hosts against bacteria. Many bacteria in turn possess pathways that provide protection against these compounds. In Escherichia coli and related bacteria, the PhoQ/PhoP signalling system is a key regulator of this antimicrobial peptide defence. Here we show that treating E. coli with sublethal concentrations of antimicrobial peptides causes cells to filament, and that this division block is controlled by the PhoQ/PhoP system. The filamentation results from increased expression of QueE, an enzyme that is part of a tRNA modification pathway but that, as we show here, also affects cell division. We also find that a functional YFP–QueE fusion localizes to the division septum in filamentous cells, suggesting QueE blocks septation through interaction with the divisome. Regulation of septation by PhoQ/PhoP may protect cells from antimicrobial peptide-induced stress or other conditions associated with high-level stimulation of this signalling system., The PhoQ/PhoP system regulates antimicrobial peptide defense in bacteria. Here the authors show that at sublethal concentrations of antimicrobial peptides, PhoPQ induces QueE, that then localizes to the divisome and blocks cell division independently of its function in queuosine biosynthesis.

Published
2016

16. Regulated stochasticity in a bacterial signaling network permits tolerance to a rapid environmental change

Author

Manuela Roggiani, Jeffrey N. Carey, Kevin S. Myers, Mark Goulian, Patricia J. Kiley, and Erin L. Mettert

Subjects
0301 basic medicine, Anaerobic respiration, Transcription, Genetic, 030106 microbiology, Population, Regulator, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Methylamines, Gene expression, medicine, Escherichia coli, Anaerobiosis, education, Promoter Regions, Genetic, Transcription factor, education.field_of_study, Binding Sites, Base Sequence, Mechanism (biology), Escherichia coli Proteins, Phosphotransferases, Phenotype, Aerobiosis, Cell biology, Up-Regulation, Oxygen, 030104 developmental biology, Periplasmic Proteins, Protein Binding, Signal Transduction, Transcription Factors
Abstract

Summary Microbial populations can maximize fitness in dynamic environments through bet hedging, a process wherein a subpopulation assumes a phenotype not optimally adapted to the present environment but well adapted to an environment likely to be encountered. Here, we show that oxygen induces fluctuating expression of the trimethylamine oxide (TMAO) respiratory system of Escherichia coli , diversifying the cell population and enabling a bet-hedging strategy that permits growth following oxygen loss. This regulation by oxygen affects the variance in gene expression but leaves the mean unchanged. We show that the oxygen-sensitive transcription factor IscR is the key regulator of variability. Oxygen causes IscR to repress expression of a TMAO-responsive signaling system, allowing stochastic effects to have a strong effect on the output of the system and resulting in heterogeneous expression of the TMAO reduction machinery. This work reveals a mechanism through which cells regulate molecular noise to enhance fitness.

Published
2018

18. A role for bacterial urease in gut dysbiosis and Crohn's disease

Author

Christopher Hoffmann, Aubrey Bailey, Abigail Lauder, Clary B. Clish, Eric Z. Chen, Andrew Lin, Kyle Bittinger, James D. Lewis, Hongzhe Li, Elliot S. Friedman, Gary D. Wu, Ramnik J. Xavier, Ting-Chin David Shen, Gloriany Rivas, Manuela Roggiani, Mark Goulian, Frederic D. Bushman, Robert N. Baldassano, Justin Scott, Jonathan Braun, Lindsey Albenberg, Lillian Chau, Alexandra Sirota-Madi, Josephine Ni, Ilana Nissim, and Marc Yudkoff

Subjects
0301 basic medicine, Urease, Gut flora, medicine.disease_cause, digestive system, Inflammatory bowel disease, Article, Microbiology, 03 medical and health sciences, Mice, 0302 clinical medicine, Bacterial Proteins, Crohn Disease, medicine, Animals, Humans, Colitis, Escherichia coli, Feces, Crohn's disease, biology, digestive, oral, and skin physiology, General Medicine, biology.organism_classification, medicine.disease, Gastrointestinal Microbiome, 030104 developmental biology, Immunology, biology.protein, Dysbiosis, 030211 gastroenterology & hepatology
Abstract

Gut dysbiosis during inflammatory bowel disease involves alterations in the gut microbiota associated with inflammation of the host gut. We used a combination of shotgun metagenomic sequencing and metabolomics to analyze fecal samples from pediatric patients with Crohn’s disease and found an association between disease severity, gut dysbiosis, and bacterial production of free amino acids. Nitrogen flux studies using 15 N in mice showed that activity of bacterial urease, an enzyme that releases ammonia by hydrolysis of host urea, led to the transfer of murine host-derived nitrogen to the gut microbiota where it was used for amino acid synthesis. Inoculation of a conventional murine host (pretreated with antibiotics and polyethylene glycol) with commensal Escherichia coli engineered to express urease led to dysbiosis of the gut microbiota, resulting in a predominance of Proteobacteria species. This was associated with a worsening of immune-mediated colitis in these animals. A potential role for altered urease expression and nitrogen flux in the development of gut dysbiosis suggests that bacterial urease may be a potential therapeutic target for inflammatory bowel diseases.

Published
2016

19. Membrane protein expression triggers chromosomal locus repositioning in bacteria

Author

Elizabeth A. Libby, Manuela Roggiani, and Mark Goulian

Subjects
Genetics, Vesicle-associated membrane protein 8, Multidisciplinary, Monosaccharide Transport Proteins, Symporters, Escherichia coli Proteins, Circular bacterial chromosome, Membrane Proteins, Chromosome, Locus (genetics), Gene Expression Regulation, Bacterial, Chromosomes, Bacterial, Biological Sciences, Biology, beta-Galactosidase, Luminescent Proteins, Microscopy, Fluorescence, Membrane protein, Start codon, Acetyltransferases, Symporter, Escherichia coli, Gene
Abstract

It has long been hypothesized that subcellular positioning of chromosomal loci in bacteria may be influenced by gene function and expression state. Here we provide direct evidence that membrane protein expression affects the position of chromosomal loci in Escherichia coli . For two different membrane proteins, we observed a dramatic shift of their genetic loci toward the membrane upon induction. In related systems in which a cytoplasmic protein was produced, or translation was eliminated by mutating the start codon, a shift was not observed. Antibiotics that block transcription and translation similarly prevented locus repositioning toward the membrane. We also found that repositioning is relatively rapid and can be detected at positions that are a considerable distance on the chromosome from the gene encoding the membrane protein (>90 kb). Given that membrane protein-encoding genes are distributed throughout the chromosome, their expression may be an important mechanism for maintaining the bacterial chromosome in an expanded and dynamic state.

Published
2012

22. Oxygen-Dependent Cell-to-Cell Variability in the Output of the Escherichia coli Tor Phosphorelay

Author

Mark Goulian and Manuela Roggiani

Subjects
education.field_of_study, Anaerobic respiration, Transcription, Genetic, Escherichia coli Proteins, Population, chemistry.chemical_element, Periplasmic space, Articles, Gene Expression Regulation, Bacterial, Biology, medicine.disease_cause, Microbiology, Oxygen, Response regulator, Biochemistry, chemistry, medicine, Escherichia coli, Signal transduction, education, Molecular Biology, Transcription factor, Signal Transduction
Abstract

Escherichia coli senses and responds to trimethylamine- N -oxide (TMAO) in the environment through the TorT-TorS-TorR signal transduction system. The periplasmic protein TorT binds TMAO and stimulates the hybrid kinase TorS to phosphorylate the response regulator TorR through a phosphorelay. Phosphorylated TorR, in turn, activates transcription of the torCAD operon, which encodes the proteins required for anaerobic respiration via reduction of TMAO to trimethylamine. Interestingly, E. coli respires TMAO in both the presence and absence of oxygen, a behavior that is markedly different from the utilization of other alternative electron acceptors by this bacterium. Here we describe an unusual form of regulation by oxygen for this system. While the average level of torCAD transcription is the same for aerobic and anaerobic cultures containing TMAO, the behavior across the population of cells is strikingly different under the two growth conditions. Cellular levels of torCAD transcription in aerobic cultures are highly heterogeneous, in contrast to the relatively homogeneous distribution in anaerobic cultures. Thus, oxygen regulates the variance of the output but not the mean for the Tor system. We further show that this oxygen-dependent variability stems from the phosphorelay. IMPORTANCE Trimethylamine- N -oxide (TMAO) is utilized by numerous bacteria as an electron acceptor for anaerobic respiration. In E. coli , expression of the proteins required for TMAO respiration is tightly regulated by a signal transduction system that is activated by TMAO. Curiously, although oxygen is the energetically preferred electron acceptor, TMAO is respired even in the presence of oxygen. Here we describe an interesting and unexpected form of regulation for this system in which oxygen produces highly variable expression of the TMAO utilization proteins across a population of cells without affecting the mean expression of these proteins. To our knowledge, this is the first reported example of a stimulus regulating the variance but not the mean output of a signaling system.

Published
2015

23. Natural variation of a sensor kinase controlling a conserved stress response pathway in Escherichia coli

Author

Srujana S. Yadavalli, Manuela Roggiani, and Mark Goulian

Subjects
0301 basic medicine, Cancer Research, Operon, Pathology and Laboratory Medicine, medicine.disease_cause, Biochemistry, Database and Informatics Methods, Fluorescence Microscopy, Nucleic Acids, Medicine and Health Sciences, Genetics (clinical), Data Management, Genetics, Escherichia Coli, Microscopy, Bacterial Genomics, biology, Kinase, Escherichia coli Proteins, Microbial Genetics, Salmonella enterica, Light Microscopy, Genomics, Hydrogen-Ion Concentration, Bacterial Pathogens, Phylogenetics, Experimental Organism Systems, Medical Microbiology, Prokaryotic Models, Pathogens, Signal transduction, Sequence Analysis, Signal Transduction, Research Article, Escherichia, Computer and Information Sciences, lcsh:QH426-470, Bioinformatics, Sequence analysis, 030106 microbiology, Sequence alignment, Microbial Genomics, DNA construction, Research and Analysis Methods, Regulon, Microbiology, 03 medical and health sciences, Model Organisms, Enterobacteriaceae, medicine, Bacterial Genetics, Evolutionary Systematics, Operons, Microbial Pathogens, Molecular Biology, Escherichia coli, Ecology, Evolution, Behavior and Systematics, Taxonomy, Evolutionary Biology, Bacteria, Gut Bacteria, Organisms, Biology and Life Sciences, Bacteriology, Gene Expression Regulation, Bacterial, DNA, biology.organism_classification, lcsh:Genetics, Molecular biology techniques, Plasmid Construction, Protein Kinases, Sequence Alignment, Transcription Factors
Abstract

Previous studies have shown that exponentially growing Escherichia coli can detect mild acidity (~pH 5.5) and, in response, synthesize enzymes that protect against severe acid shock. This adaptation is controlled by the EvgS/EvgA phosphorelay, a signal transduction system present in virtually every E. coli isolate whose genome has been sequenced. Here we show that, despite this high level of conservation, the EvgS/EvgA system displays a surprising natural variation in pH-sensing capacity, with some strains entirely non-responsive to low pH stimulus. In most cases that we have tested, however, activation of the EvgA regulon still confers acid resistance. From analyzing selected E. coli isolates, we find that the natural variation results from polymorphisms in the sensor kinase EvgS. We further show that this variation affects the pH response of a second kinase, PhoQ, which senses pH differently from the closely related PhoQ in Salmonella enterica. The within-species diversification described here suggests EvgS likely responds to additional input signals that may be correlated with acid stress. In addition, this work highlights the fact that even for highly conserved sensor kinases, the activities identified from a subset of isolates may not necessarily generalize to other members of the same bacterial species., Author summary Bacteria employ a class of proteins, sensor kinases, to sense environmental cues and initiate cellular responses through phosphorylation of partner response regulator proteins. Individual kinases are generally assumed to have the same sensory activity across members of a bacterial species. In this work, we report an unexpected counterexample in which the well-established capacity of the kinase EvgS to sense mild acidity is limited to a subset of Escherichia coli isolates. Despite this natural variation, EvgS activation still confers resistance to acid stress in strains that have lost EvgS pH-sensing activity. Thus, most E. coli share a conserved output of the Evg system but do not require identical sensory functions. This work highlights the potential for significant functional divergence of a sensor kinase within a species and also indicates that there are additional input signals for the highly conserved EvgS protein.

Published
2017

24. A Role for Bacterial Urease in Crohn's Disease and Gut Dysbiosis

Author

Eric Z. Chen, Marc Yudkoff, Frederic D. Bushman, Josephine Ni, Ramnik J. Xavier, Ting-Chin David Shen, Mark Goulian, Jonathan Braun, Aubrey Bailey, Clary B. Clish, James D. Lewis, Manuela Roggiani, Hongzhe Li, Robert N. Baldassano, Elliot S. Friedman, Lindsey Albenberg, Lillian Chau, Alexandra Sirota-Madi, and Gary D. Wu

Subjects
0301 basic medicine, Crohn's disease, Hepatology, Urease, Gastroenterology, Biology, medicine.disease, Microbiology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, biology.protein, medicine, 030211 gastroenterology & hepatology, Gut dysbiosis
Published
2017

25. Toxoids of Streptococcal Pyrogenic Exotoxin A Are Protective in Rabbit Models of Streptococcal Toxic Shock Syndrome

Author

Subramonia Pillai, Patrick M. Schlievert, Douglas H. Ohlendorf, Jennifer Stoehr, Manuela Roggiani, Yury V. Matsuka, and Stephen B. Olmsted

Subjects
Streptococcus pyogenes, Immunology, Receptors, Antigen, T-Cell, Exotoxins, Mutagenesis (molecular biology technique), chemical and pharmacologic phenomena, Major histocompatibility complex, medicine.disease_cause, Microbiology, Lethal Dose 50, Mice, Bacterial Proteins, Streptococcal Infections, medicine, Superantigen, Animals, Humans, Mice, Inbred BALB C, Superantigens, biology, Streptococcus, Toxin, T-cell receptor, Histocompatibility Antigens Class II, Membrane Proteins, Toxoids, Shock, Septic, Infectious Diseases, Microbial Immunity and Vaccines, Mutation, biology.protein, Parasitology, Rabbits, Exotoxin
Abstract

Streptococcal pyrogenic exotoxins (SPEs) are superantigens that have been implicated in causing streptococcal toxic shock syndrome (STSS). Most notably, SPE serotype A is made by nearly all M-protein serotype 1 and 3 streptococci, the M types most associated with the illness (these strains contain one or more other SPEs, and those proteins are likely also to contribute to disease). We have prepared double-, triple-, and hexa-amino-acid mutants of SPE A by PCR and other mutagenesis procedures. The sites chosen for mutation were solvent-exposed residues thought to be important for T-cell receptor (TCR) or major histocompatibility complex (MHC) class II interaction. These mutants were nonsuperantigenic for human peripheral blood mononuclear cells and rabbit and mouse splenocytes and were nonlethal in two rabbit models of STSS. In addition, these mutants stimulated protective antibody responses. Interestingly, mutants that altered toxin binding to MHC class II were more immunogenic than mutants altering TCR binding. Collectively, these studies indicate that multiple-site mutants of SPE A are toxoids that may have use in protecting against the toxin's effects in STSS.

Published
2000

26. Pyrogenic Toxin Superantigen Site Specificity in Toxic Shock Syndrome and Food Poisoning in Animals

Author

David T. Mitchell, Scott D. Callantine, Patrick M. Schlievert, Ingrid Sadler, Manuela Roggiani, Gregory A. Bohach, Douglas H. Ohlendorf, and Lynn M. Jablonski

Subjects
Models, Molecular, genetic structures, Bacterial Toxins, Molecular Sequence Data, Immunology, Exotoxins, Enterotoxin, Biology, medicine.disease_cause, Microbiology, Enterotoxins, Bacterial Proteins, Streptococcal Infections, medicine, Superantigen, Animals, Amino Acid Sequence, Host Response and Inflammation, Superantigens, Food poisoning, Sequence Homology, Amino Acid, Pyrogens, Toxin, Membrane Proteins, Toxic shock syndrome, bacterial infections and mycoses, medicine.disease, Shock, Septic, Staphylococcal Food Poisoning, Infectious Diseases, Staphylococcus aureus, Streptococcus pyogenes, Parasitology, Rabbits, Macaca nemestrina
Abstract

Staphylococcus aureusandStreptococcus pyogenesexpress pyrogenic toxin superantigens (PTSAgs) that are associated with toxic shock syndrome (TSS) and staphylococcal food poisoning (SFP). Most PTSAgs cause TSS in deep-tissue infections, whereas only TSS toxin 1 (TSST-1) is associated with menstrual, vaginal TSS. In contrast, SFP has been linked only with staphylococcal enterotoxins (SEs). Because of the differential abilities of PTSAgs to cause systemic or localized symptoms in a site-dependent manner, the present study was undertaken to assess the toxins' abilities to cross mucosal barriers. The activity of three PTSAgs when delivered orally, vaginally, or intravenously to rabbits and orally to monkeys was investigated. TSST-1 induced shock via all three routes in rabbits. Although active when administered intravenously, SEC1 and streptococcal pyrogenic exotoxin A (SPEA) did not cause symptoms when administered orally or vaginally. Only SEC1 induced emesis in the monkey feeding assay. TSST-1, albeit less stable than SEC1 and SPEA to pepsin, induced diarrhea in monkeys. Our results may explain the unique association of TSST-1 with menstrual TSS and why SPEA is only rarely associated with TSS after pharyngitis, despite being highly associated with TSS after subcutaneous infections. Finally, our studies indicate that enterotoxicity in SFP is not the result of superantigenicity.

Published
2000

27. Analysis of toxicity of streptococcal pyrogenic exotoxin A mutants

Author

Bettina A. B. Leonard, Manuela Roggiani, Patrick M. Schlievert, and Jennifer Stoehr

Subjects
Streptococcus pyogenes, Immunology, Exotoxins, chemical and pharmacologic phenomena, Biology, Lymphocyte Activation, medicine.disease_cause, Microbiology, Mice, Bacterial Proteins, Drug Stability, In vivo, medicine, Superantigen, Animals, Superantigens, Pyrogens, Toxin, Membrane Proteins, Interleukin, hemic and immune systems, Biological activity, Shock, Septic, In vitro, Infectious Diseases, Mutagenesis, Site-Directed, Parasitology, Rabbits, Exotoxin, Research Article
Abstract

Streptococcal pyrogenic exotoxin A (SPE A) is secreted by some strains of Streptococcus pyogenes and is strongly associated with streptococcal toxic shock syndrome (STSS), a severe and often fatal illness. SPE A possesses a number of biological properties, some of which are shared with a group of exotoxins of streptococcal and staphylococcal origins, the pyrogenic toxin superantigens (PTSAgs). SPE A's most extensively studied property is superantigenicity. Superantigenic activation of T cells and monocytes stimulates the release of cytokines such as tumor necrosis factors alpha and beta, interleukin 1, and gamma interferon. These endogenous mediators are considered to be the primary cause of capillary leak, hypotension, and shock, the most severe manifestations of STSS. However, several studies have suggested that other properties of SPE A, such as ability to greatly enhance host susceptibility to endotoxin and ability to interact directly with endothelial cells, may play substantial roles in the syndrome. In this work we generated single- and double-site mutations of SPE A at residues K16, N20, C87, C90, C98, K157, S195, N20/C98, and N20/K157. The mutant SPE A's were analyzed in vivo for their lethal activity and in vitro for their superantigenic ability. Our results indicate that SPE A's ability to induce lethality and endotoxin enhancement does not require superantigenicity, and conversely superantigenicity does not necessarily lead to lethality. Thus, these properties and their relative contributions to the onset of hypotension and shock may be separable. Furthermore, evidence is presented that certain mutant toxins may be suitable for use as vaccine toxoids.

Published
1997

29. Purification of Streptococcal Pyrogenic Exotoxin A

Author

Manuela Roggiani and Patrick M. Schlievert

Subjects
Chemistry, Toxin, Erythrogenic toxin, Clostridium difficile toxin A, Virulence, medicine.disease_cause, medicine.disease, Group A, Microbiology, stomatognathic diseases, Superantigen, medicine, Scarlet fever, Secretion
Abstract

Group A streptococci secrete a variety of molecules, many of which are recognized as virulence factors important in the establishment of streptococcal infections. Among these extracellular products is streptococcal pyrogenic exotoxin A (SPE A, scarlet fever toxin A, erythrogenic toxin A) (1). Other SPEs include toxin serotypes B and C (1), streptococcal superantigen (SSA) (2), and SPE F (mitogenic factor) (3,4). Combinations of these toxins are believed to be important in streptococcal toxic shock syndrome. The latter two molecules will not be discussed in this chapter, but methods utilized to purify SPEs A-C also may be used to purify SSA and SPE F.

Published
2003

30. Structure of streptococcal pyrogenic exotoxin A reveals a novel metal cluster

Author

Gregory M. Vath, Patrick M. Schlievert, Manuela Roggiani, Cathleen A. Earhart, and Douglas H. Ohlendorf

Subjects
Models, Molecular, Cadmium, biology, Toxin, Stereochemistry, Ligand, Protein Conformation, chemistry.chemical_element, Exotoxins, Membrane Proteins, Zinc, medicine.disease_cause, biology.organism_classification, Biochemistry, Protein structure, chemistry, Tetramer, Bacterial Proteins, Metals, Spea, Streptococcus pyogenes, medicine, Molecular Biology, Research Article
Abstract

The streptococcal pyrogenic toxins A, B, and C (SPEA, SPEB, and SPEC) are responsible for the fever, rash, and other toxicities associated with scarlet fever and streptococcal toxic shock syndrome. This role, together with the ubiquity of diseases caused by Streptococcus pyogenes, have prompted structural analyses of SPEA by several groups. Papageorgiou et al. (1999) have recently reported the structure of SPEA crystallized in the absence of zinc. Zinc has been shown to be important in the ability of some staphylococcal and streptococcal toxins to stimulate proliferation of CD4+ T-cells. Since cadmium is more electron dense than zinc and typically binds interchangeably, we grew crystals in the presence of 10 mM CdCl2. Crystals have been obtained in three space groups, and the structure in the P2(1)2(1)2(1) crystal form has been refined to 1.9 A resolution. The structural analysis revealed an identical tetramer as well as a novel tetrahedral cluster of cadmium in all three crystal forms on a disulfide loop encompassing residues 87-98. No cadmium was bound at the site homologous to the zinc site in staphylococcal enterotoxins C (SECs) despite the high structural homology between SPEA and SECs. Subsequent soaking of crystals grown in the presence of cadmium in 10 mM ZnCl2 showed that zinc binds in this site (indicating it can discriminate between zinc and cadmium ions) using the three ligands (Asp77, His106, and His110) homologous to the SECs plus a fourth ligand (Glu33).

Published
2000

31. Isolation and preliminary characterization of plasmid in Bacillus licheniformis strain MP3

Author

Pier Luigi Manachini, Carlo Parini, Manuela Roggiani, and Maria Grazia Fortina

Subjects
Plasmid preparation, Restriction site, Plasmid, Restriction map, Strain (chemistry), Cloning vector, Bacillus licheniformis, Biology, Molecular cloning, biology.organism_classification, Applied Microbiology and Biotechnology, Molecular biology
Abstract

A restriction analysis of a single covalently closed circular plasmid isolated from Bacillus licheniformis strain MP3 was performed. A restriction map of the 6·44 kb plasmid is presented. The existence of genetic markers such as antibiotics and heavy metal ions resistance was investigated. The availability of two single restriction sites and the stability of this plasmid make it ideal for development as a cloning vector.

Published
1989

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