Your search keyword '"Heino M"' showing total 17 results

1. Comparative Molecular and Immunoregulatory Analysis of Extracellular Vesicles from Candida albicans and Candida auris

Author

Rafaela F. Amatuzzi, Daniel Zamith-Miranda, Radames J. B. Cordero, Heino M. Heyman, Marcio L. Rodrigues, Joshua D. Nosanchuk, Leonardo Nimrichter, Lysangela R. Alves, Ernesto S. Nakayasu, Sneha P. Couvillion, and Arturo Casadevall

Subjects

Physiology, Virulence, Context (language use), Proteomics, Biochemistry, Microbiology, Transcriptome, Candida albicans, Genetics, Molecular Biology, Ecology, Evolution, Behavior and Systematics, biology, fungal pathogenesis, Effector, Pathogenic fungus, Candida auris, multi-omics, biology.organism_classification, candidiasis, Corpus albicans, QR1-502, Computer Science Applications, Modeling and Simulation, extracellular vesicles, Intracellular, Research Article

Abstract

Candida auris is a recently described multidrug-resistant pathogenic fungus that is increasingly responsible for health care-associated outbreaks across the world. Bloodstream infections of this fungus cause death in up to 70% of cases. Aggravating this scenario, the disease-promoting mechanisms of C. auris are poorly understood. Fungi release extracellular vesicles (EVs) that carry a broad range of molecules, including proteins, lipids, carbohydrates, pigments, and RNA, many of which are virulence factors. Here, we carried out a comparative molecular characterization of C. auris and Candida albicans EVs and evaluated their capacity to modulate effector mechanisms of host immune defense. Using proteomics, lipidomics, and transcriptomics, we found that C. auris released EVs with payloads that were significantly different from those of EVs released by C. albicans. EVs released by C. auris potentiated the adhesion of this yeast to an epithelial cell monolayer, while EVs from C. albicans had no effect. C. albicans EVs primed macrophages for enhanced intracellular yeast killing, whereas C. auris EVs promoted survival of the fungal cells. Moreover, EVs from both C. auris and C. albicans induced the activation of bone marrow-derived dendritic cells. Together, our findings show distinct profiles and properties of EVs released by C. auris and by C. albicans and highlight the potential contribution of C. auris EVs to the pathogenesis of this emerging pathogen. IMPORTANCECandida auris is a recently described multidrug-resistant pathogenic fungus that is responsible for outbreaks across the globe, particularly in the context of nosocomial infections. Its virulence factors and pathogenesis are poorly understood. Here, we tested the hypothesis that extracellular vesicles (EVs) released by C. auris are a disease-promoting factor. We describe the production of EVs by C. auris and compare their biological activities against those of the better-characterized EVs from C. albicans. C. auris EVs have immunoregulatory properties, of which some are opposite those of C. albicans EVs. We also explored the cargo and structural components of those vesicles and found that they are remarkably distinct compared to EVs from C. auris’s phylogenetic relative Candida albicans.

Published

2021

2. Anti-HIV-1 activity of quinic acid isolated from Helichrysum mimetes using NMR-based metabolomics and computational analysis

Author

Simin Emamzadeh Yazdi, Thomas Klimkait, J.J.M. Meyer, Heino M. Heyman, Gerhard Prinsloo, and Carel Basson Oosthuizen

Subjects

chemistry.chemical_classification, Chromatography, biology, Plant Science, Quinic acid, biology.organism_classification, chemistry.chemical_compound, Enzyme, chemistry, Drug control, Docking (molecular), Helichrysum, Proton NMR, Mimetes, Dichloromethane

Abstract

Helichrysum species are widely used in traditional medicine with potential against infectious diseases. Extraction of the aerial parts of 32 Helichrysum species was done using polar (methanol:water (1:1)) and non-polar (hexane, dichloromethane and acetone) solvent systems. Anti-human immunodeficiency virus (HIV) bioassays revealed that polar extracts of H. mimetes and H. chrysargyrum (2.5 μg/mL), polar and non-polar extracts of H. cephaloideum (25 μg/mL) and polar and non-polar extracts of H. zeyheri, H. setosum, H. platypterum and H. kraussii at (2.5 μg/mL), had greater than 90% inhibitory activity. The polar extract of H. mimetes (100 μg/mL) exhibited 55.93% reverse transcriptase (RT) inhibition as a possible indication of the mechanism of action. Proton NMR spectra of the polar extracts exhibited the presence of aromatic compounds and carbohydrate moieties. Principal component analysis (PCA) of the polar extracts showed clustering related to the activity of the extracts with good predictability scores (Q2 > 0.5). However, orthogonal projections to latent structures discriminant analysis (OPLS-DA) predictability of the model was low based on the Q2 at approximately 0.25. Quinic acid (QA) isolated from H. mimetes showed promising anti-RT activity (IC50 = 53.82 μg/mL) comparable to the positive drug control, doxorubicin (IC50 = 40.31 μg/mL). A molecular docking study revealed the probable binding site and conformation of QA within cavity 4, with a docking score of − 8.03. The docking score of doxorubicin within cavity 4 was − 7.87. These are the first reports of QA's HIV-1-RT activity, as well as doxorubicin's docking characteristics on this enzyme.

Published

2019

3. 1H NMR-based metabolomics of antimalarial plant species traditionally used by Vha-Venda people in Limpopo Province, South Africa and isolation of antiplasmodial compounds

Author

Heino M. Heyman, François Senejoux, J.J. Marion Meyer, and M. Johanna Bapela

Subjects

Pharmacology, 0303 health sciences, biology, Traditional medicine, Iridoid, Vangueria infausta, medicine.drug_class, Friedelin, Tabernaemontana elegans, biology.organism_classification, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Metabolomics, chemistry, Phytochemical, 030220 oncology & carcinogenesis, Drug Discovery, medicine, Medicinal plants, Vangueria, 030304 developmental biology

Abstract

Ethnopharmacological relevance The Vha-Venda people living in rural areas of Limpopo Province of South Africa regularly use traditional plant-based medicines to treat malaria. In our earlier publication, twenty indigenous plant species used to treat malaria or its symptoms by Vha-Venda people were evaluated for antiplasmodial activity. The main objective of the current study was to assess the robustness of NMR-based metabolomics in discriminating classes of secondary compounds that are responsible for the observed antimalarial activity and the isolation of antiplasmodial compounds. Materials and methods Twenty dichloromethane extracts were reconstituted in CDCl3, subjected to 1H NMR-based metabolomic analysis on a Varian 600 MHz spectrometer and the acquired 1H NMR spectra were then evaluated collectively using multivariate data analysis (MDA). Principal Component Analysis (PCA) and Orthogonal Projections to Latent Structures–Discriminant Analysis (OPLS-DA) were used to ‘globally’ discern antiplasmodial profiles. A contribution plot was then generated from the OPLS-DA scoring plot in an attempt to determine the classes of compounds that are responsible for the observed grouping. Further phytochemical analyses were conducted on the lipophilic extracts of Tabernaemontana elegans and Vangueria infausta subsp. infausta. These best candidates were fractionated, purified and their isolated compounds identified based on conventional chromatographic and spectroscopic techniques. Results The PCA did not separate the acquired profiles according to the detected antiplasmodial bioactivity. Application of a supervised OPLS-DA on the 1H NMR profiles resulted in a discrimination pattern that could be correlated to the observed antimalarial bioactivity. A contribution plot generated from the OPLS-DA scoring plot illustrated the classes of compounds responsible for the observed grouping. Prominent peaks were observed in the aromatic, sugar-based/N-containing and aliphatic spectral regions of the contribution plot. Two known indole alkaloids were isolated from T. elegans, and identified as tabernaemontanine (IC50 = 12.0 ± 0.8 µM) and dregamine (IC50 = 62.0 ± 2.4 µM). Friedelin (IC50 = 7.20 ± 0.5 µM) and morindolide (IC50 = 107.1 ± 0.6 µM) were isolated from V. infausta subsp. infausta. This is the first report of the rare iridoid lactone, morindolide's antimalarial activity. While these two compounds have been previously identified, this is the first account of their occurrence in the genus Vangueria. Conclusion The study illustrated the potential of NMR-based metabolomics in discriminating classes of compounds that may be attributed to antiplasmodial activity. Additionally, the study demonstrated the potential of discovering novel antiplasmodial scaffolds from medicinal plants and the rationale for the bioprospecting antimalarial plant species used by Vha-Venda people.

Published

2019

4. Cryptococcus neoformans Secretes Small Molecules That Inhibit IL-1β Inflammasome-Dependent Secretion

Author

Joshua D. Nosanchuk, Aldo Henrique Tavares, Patrícia Albuquerque, Paulo Henrique de Holanda Veloso Janior, Robin C. May, Carolina Coelho, Arturo Casadevall, Pedro Henrique Viana Saavedra, Raffael Júnio Araújo de Castro, Ernesto S. Nakayasu, Clara Luna Marina, Pedro Henrique Bürgel, Stephan Alberto Machado de Oliveira, Heino M. Heyman, Anamélia Lorenzetti Bocca, and Radames J. B. Cordero

Subjects

0301 basic medicine, Article Subject, Phagocytosis, Immunology, Virulence, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Pathology, medicine, RB1-214, Secretion, Cryptococcus neoformans, biology, Chemistry, Pyroptosis, Inflammasome, Cell Biology, biology.organism_classification, medicine.disease, Antibody opsonization, 030104 developmental biology, Cryptococcosis, 030215 immunology, medicine.drug, Research Article

Abstract

Cryptococcus neoformans is an encapsulated yeast that causes disease mainly in immunosuppressed hosts. It is considered a facultative intracellular pathogen because of its capacity to survive and replicate inside phagocytes, especially macrophages. This ability is heavily dependent on various virulence factors, particularly the glucuronoxylomannan (GXM) component of the polysaccharide capsule. Inflammasome activation in phagocytes is usually protective against fungal infections, including cryptococcosis. Nevertheless, recognition of C. neoformans by inflammasome receptors requires specific changes in morphology or the opsonization of the yeast, impairing proper inflammasome function. In this context, we analyzed the impact of molecules secreted by C. neoformans B3501 strain and its acapsular mutant Δcap67 in inflammasome activation in an in vitro model. Our results showed that conditioned media derived from B3501 was capable of inhibiting inflammasome-dependent events (i.e., IL-1β secretion and LDH release via pyroptosis) more strongly than conditioned media from Δcap67, regardless of GXM presence. We also demonstrated that macrophages treated with conditioned media were less responsive against infection with the virulent strain H99, exhibiting lower rates of phagocytosis, increased fungal burdens, and enhanced vomocytosis. Moreover, we showed that the aromatic metabolite DL-Indole-3-lactic acid (ILA) and DL-p-Hydroxyphenyllactic acid (HPLA) were present in B3501’s conditioned media and that ILA alone or with HPLA is involved in the regulation of inflammasome activation by C. neoformans. These results were confirmed by in vivo experiments, where exposure to conditioned media led to higher fungal burdens in Acanthamoeba castellanii culture as well as in higher fungal loads in the lungs of infected mice. Overall, the results presented show that conditioned media from a wild-type strain can inhibit a vital recognition pathway and subsequent fungicidal functions of macrophages, contributing to fungal survival in vitro and in vivo and suggesting that secretion of aromatic metabolites, such as ILA, during cryptococcal infections fundamentally impacts pathogenesis.

Published

2020

5. Controls on Soil Organic Matter Degradation and Subsequent Greenhouse Gas Emissions Across a Permafrost Thaw Gradient in Northern Sweden

Author

Malak M. Tfaily, Heino M. Heyman, Roya AminiTabrizi, J. Fudyma, Virginia I. Rich, Scott R. Saleska, Rachel M. Wilson, Jeffrey P. Chanton, and S. B. Hodgkins

Subjects

chemistry.chemical_classification, Biogeochemical cycle, geography, geography.geographical_feature_category, Peat, fen, biology, Soil organic matter, Permafrost, biology.organism_classification, Sphagnum, Humus, chemistry, bog, soil organic matter, Environmental chemistry, General Earth and Planetary Sciences, Environmental science, lcsh:Q, Organic matter, lcsh:Science, Bog, peatlands, permafrost, mass spectrometry

Abstract

Warming-induced permafrost thaw could enhance microbial decomposition of previously stored soil organic matter (SOM) to carbon dioxide (CO2) and methane (CH4), one of the most significant potential feedbacks from terrestrial ecosystems to the atmosphere in a changing climate. The environmental parameters regulating microbe-organic matter interactions and greenhouse gas (GHG) emissions in northern permafrost peatlands are however still largely unknown. The objective of this work is to understand controls on SOM degradation and its impact on porewater GHG concentrations across the Stordalen Mire, a thawing peat plateau in Northern Sweden. Here, we applied high-resolution mass spectrometry to characterize SOM molecular composition in peat soil samples from the active layers of a Sphagnum-dominated bog and rich fen sites in the Mire. Microbe-organic matter interactions and porewater GHG concentrations across the thaw gradient were controlled by aboveground vegetation and soil pH. An increasingly high abundance of reduced organic compounds experiencing greater humification rates due to enhanced microbial activity were observed with increasing thaw, in parallel with higher CH4 and CO2 porewater concentrations. Bog SOM however contained more Sphagnum-derived phenolics, simple carbohydrates, and organic- acids. The low degradation of bog SOM by microbial communities, the enhanced SOM transformation by potentially abiotic mechanisms, and the accumulation of simple carbohydrates in the bog sites could be attributed in part to the low pH conditions of the system associated with Sphagnum mosses. We show that Gibbs free energy of C half reactions based on C oxidation state for OM can be used as a quantifiable measure for OM decomposability and quality to enhance current biogeochemical models to predict C decomposition rates. We found a direct association between OM chemical diversity and δ13C-CH4 in peat porewater; where higher substrate diversity was positively correlated with enriched δ13C-CH4 in fen sites. Oxidized sulfur-containing compounds, produced by Sphagnum, were further hypothesized to control GHG emissions by acting as electron acceptors for a sulfate-reducing electron transport chain, inhibiting methanogenesis in peat bogs. These results suggest that warming-induced permafrost thaw might increase organic matter lability, in subset of sites that become wetlands, and shift biogeochemical processes toward faster decomposition with an increasing proportion of carbon released as CH4.

Published

2020

6. Media matters! Alterations in the loading and release of Histoplasma capsulatum extracellular vesicles in response to different nutritional milieus

Author

Daniel Zamith, Ernesto S. Nakayasu, Levi G. Cleare, Sneha P. Couvillion, Marcio L. Rodrigues, Leonardo Nimrichter, Heino M. Heyman, and Joshua D. Nosanchuk

Subjects

Immunology, Histoplasma, Virulence, chemical and pharmacologic phenomena, Biology, Proteomics, Microbiology, Histoplasma capsulatum, complex mixtures, Histoplasmosis, Article, Fungal Proteins, 03 medical and health sciences, Extracellular Vesicles, fluids and secretions, Virology, parasitic diseases, medicine, Secretion, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, 030306 microbiology, Nutrients, biology.organism_classification, medicine.disease, bacterial infections and mycoses, Culture Media, Enzyme, chemistry, Pneumonia (non-human), Dimorphic fungus

Abstract

Histoplasma capsulatum is a dimorphic fungus that most frequently causes pneumonia, but can also disseminate and proliferate in diverse tissues. Histoplasma capsulatum has a complex secretion system that mediates the release of macromolecule-degrading enzymes and virulence factors. The formation and release of extracellular vesicles (EVs) are an important mechanism for non-conventional secretion in both ascomycetes and basidiomycetes. Histoplasma capsulatum EVs contain diverse proteins associated with virulence and are immunologically active. Despite the growing knowledge of EVs from H. capsulatum and other pathogenic fungi, the extent that changes in the environment impact the sorting of organic molecules in EVs has not been investigated. In this study, we cultivated H. capsulatum with distinct culture media to investigate the potential plasticity in EV loading in response to differences in nutrition. Our findings reveal that nutrition plays an important role in EV loading and formation, which may translate into differences in biological activities of these fungi in various fluids and tissues.

Published

2019

7. Untargeted metabolomic profiling of Sphagnum fallax reveals novel antimicrobial metabolites

Author

David W. Hoyt, J. Fudyma, Jason Toyoda, Rosalie K. Chu, H. Gieschen, Thomas O. Metz, Malak M. Tfaily, Jennifer E. Kyle, Nikola Tolić, Jamee Lyon, Roya AminiTabrizi, Heino M. Heyman, and Nancy J. Hess

Subjects

chemistry.chemical_classification, Ecology, biology, Chemistry, Metabolite, Botany, Sphagnum fallax, Plant Science, Lipidome, biology.organism_classification, Antimicrobial, metabolomics, Biochemistry, Genetics and Molecular Biology (miscellaneous), Sphagnum, chemistry.chemical_compound, Metabolomics, QK1-989, Lipidomics, antimicrobial metabolites, lipidomics, Organic matter, fungal metabolites, Ecology, Evolution, Behavior and Systematics

Abstract

Sphagnum mosses dominate peatlands by employing harsh ecosystem tactics to prevent vascular plant growth and microbial degradation of these large carbon stores. Knowledge about Sphagnum‐produced metabolites, their structure and their function, is important to better understand the mechanisms, underlying this carbon sequestration phenomenon in the face of climate variability. It is currently unclear which compounds are responsible for inhibition of organic matter decomposition and the mechanisms by which this inhibition occurs. Metabolite profiling of Sphagnum fallax was performed using two types of mass spectrometry (MS) systems and 1H nuclear magnetic resonance spectroscopy (1H NMR). Lipidome profiling was performed using LC‐MS/MS. A total of 655 metabolites, including one hundred fifty‐two lipids, were detected by NMR and LC‐MS/MS—329 of which were novel metabolites (31 unknown lipids). Sphagum fallax metabolite profile was composed mainly of acid‐like and flavonoid glycoside compounds, that could be acting as potent antimicrobial compounds, allowing Sphagnum to control its environment. Sphagnum fallax metabolite composition comparison against previously known antimicrobial plant metabolites confirmed this trend, with seventeen antimicrobial compounds discovered to be present in Sphagnum fallax, the majority of which were acids and glycosides. Biological activity of these compounds needs to be further tested to confirm antimicrobial qualities. Three fungal metabolites were identified providing insights into fungal colonization that may benefit Sphagnum. Characterizing the metabolite profile of Sphagnum fallax provided a baseline to understand the mechanisms in which Sphagnum fallax acts on its environment, its relation to carbon sequestration in peatlands, and provide key biomarkers to predict peatland C store changes (sequestration, emissions) as climate shifts.

Published

2019

8. Multi-omics Signature of Candida auris, an Emerging and Multidrug-Resistant Pathogen

Author

Levi G. Cleare, Ernesto S. Nakayasu, Attila Gácser, Erin L. Bredeweg, Sneha P. Couvillion, Leonardo Nimrichter, Joshua D. Nosanchuk, Daniel Zamith-Miranda, Geremy Clair, and Heino M. Heyman

Subjects

0301 basic medicine, Molecular Biology and Physiology, Physiology, 030106 microbiology, Virulence, Drug resistance, Biochemistry, Microbiology, Carbon utilization, 03 medical and health sciences, fluconazole, Genetics, Candida albicans, Molecular Biology, Pathogen, Ecology, Evolution, Behavior and Systematics, biology, Pathogenic fungus, Candida auris, antifungal resistance, multi-omics, biology.organism_classification, Corpus albicans, QR1-502, 3. Good health, Computer Science Applications, 030104 developmental biology, Modeling and Simulation, Research Article

Abstract

Candida auris was first described in Japan in 2009 and has now been the cause of significant outbreaks across the globe. The high number of isolates that are resistant to one or more antifungals, as well as the high mortality rates from patients with bloodstream infections, has attracted the attention of the medical mycology, infectious disease, and public health communities to this pathogenic fungus. In the current work, we performed a broad multi-omics approach on two clinical isolates isolated in New York, the most affected area in the United States and found that the omic profile of C. auris differs significantly from C. albicans. In addition to our insights into C. auris carbon utilization and lipid and protein content, we believe that the availability of these data will enhance our ability to combat this rapidly emerging pathogenic yeast., Candida auris is a recently described pathogenic fungus that is causing invasive outbreaks on all continents. The fungus is of high concern given the numbers of multidrug-resistant strains that have been isolated in distinct sites across the globe. The fact that its diagnosis is still problematic suggests that the spreading of the pathogen remains underestimated. Notably, the molecular mechanisms of virulence and antifungal resistance employed by this new species are largely unknown. In the present work, we compared two clinical isolates of C. auris with distinct drug susceptibility profiles and a Candida albicans reference strain using a multi-omics approach. Our results show that, despite the distinct drug resistance profile, both C. auris isolates appear to be very similar, albeit with a few notable differences. However, compared to C. albicans both C. auris isolates have major differences regarding their carbon utilization and downstream lipid and protein content, suggesting a multifactorial mechanism of drug resistance. The molecular profile displayed by C. auris helps to explain the antifungal resistance and virulence phenotypes of this new emerging pathogen. IMPORTANCE Candida auris was first described in Japan in 2009 and has now been the cause of significant outbreaks across the globe. The high number of isolates that are resistant to one or more antifungals, as well as the high mortality rates from patients with bloodstream infections, has attracted the attention of the medical mycology, infectious disease, and public health communities to this pathogenic fungus. In the current work, we performed a broad multi-omics approach on two clinical isolates isolated in New York, the most affected area in the United States and found that the omic profile of C. auris differs significantly from C. albicans. In addition to our insights into C. auris carbon utilization and lipid and protein content, we believe that the availability of these data will enhance our ability to combat this rapidly emerging pathogenic yeast.

Published

2019

9. Cryptococcus neoformans secretes small molecules that inhibit IL-1β inflammasome-dependent secretion

Author

Robin C. May, Patrícia Albuquerque, Heino M. Heyman, P. H. Holanda, Aldo Henrique Tavares, Joshua D. Nosanchuk, P. H. V. Saavedra, R. d. A. Castro, Arturo Casadevall, Carolina Coelho, E. Nakayasu, Clara Luna Marina, Radames J. B. Cordero, Anamélia Lorenzetti Bocca, and P. H. Bürgel

Subjects

Cryptococcus neoformans, biology, Chemistry, Intracellular parasite, Pyroptosis, Inflammasome, medicine.disease, biology.organism_classification, Microbiology, Antibody opsonization, Immune system, Cryptococcosis, medicine, Macrophage, medicine.drug

Abstract

Cryptococcus neoformansis an encapsulated yeast that causes disease mainly in immunosuppressed hosts. It is considered a facultative intracellular pathogen because of its capacity to survive and replicate inside phagocytes, especially macrophages. This capacity is heavily dependent on various virulence factors, particularly the glucuronoxylomannan (GXM) component of the polysaccharide capsule, that render the non- or poorly-activated macrophage ineffective against phagocytosed yeast. Strategies utilized by macrophages to prevent this scenario include pyroptosis (a rapid highly inflammatory cell death) and vomocytosis (the expulsion of the pathogen from the intracellular environment without lysis). Inflammasome activation in phagocytes is usually protective against fungal infections, including cryptococcosis. Nevertheless, recognition ofC. neoformansby inflammasome receptors requires specific changes in morphology or the opsonization of the yeast, impairing a proper inflammasome function. In this context, we analyzed the impact of molecules secreted byC. neoformansB3501 strain and its acapsular mutantΔcap67in an inflammasome activationin vitromodel. Our results showed that conditioned media derived from B3501 was capable of inhibiting inflammasome dependent events (i. e. IL-1β secretion and LDH release via pyroptosis) more strongly than conditioned media fromΔcap67, regardless of GXM presence. We also demonstrated that macrophages treated with conditioned media were less responsive against infection with the virulent strain H99, exhibiting lower rates of phagocytosis, increased fungal burdens and enhanced vomocytosis. Moreover, we showed that the aromatic metabolite DL-Indole-3-lactic acid (ILA) was present in B3501’s conditioned media and that this fungal metabolite is involved in the regulation of inflammasome activation byC. neoformans. Overall, the results presented show that conditioned media from a wild-type strain can inhibit an important recognition pathway and subsequent fungicidal functions of macrophages, contributing to fungal survivalin vitroand suggesting that this serves as an important role for secreted molecules during cryptococcal infections.Author’s SummaryCryptococcus neoformansis the agent of cryptococcal meningitis, a disease that can be life-threatening in immunocompromised hosts such as those infected with HIV. The infection thrives in hosts that poorly activate their immune system, mainly because of the yeast’s ability to survive inside macrophages and migrate towards the central nervous system. Emerging data indicate that cryptococci modulate the host immune response, but the underlying mechanisms remain largely uncharacterized. Here we show that secreted molecules from a wild-type strain ofC. neoformansimpair inflammatory responses driven by inflammasome activation, which in turn impact the macrophage antifungal activity. We further show that this inhibition does not involve GXM, the main constituent of the fungal capsule, but rather is partially dependent on DL-Indole-3-lactic acid (ILA), a metabolite not previously implicated in fungal virulence.

Published

2019

10. Candida auris: multi-omics signature of an emerging and multidrug-resistant pathogen

Author

Attila Gácser, Leonardo Nimrichter, Geremy Clair, Levi G. Cleare, Heino M. Heyman, Joshua D. Nosanchuk, Daniel Zamith-Miranda, Ernesto S. Nakayasu, Erin L. Bredeweg, and Sneha P. Couvillion

Subjects

0303 health sciences, biology, 030306 microbiology, Virulence, Drug resistance, Pathogenic fungus, biology.organism_classification, Corpus albicans, 3. Good health, Carbon utilization, Microbiology, 03 medical and health sciences, Candida auris, Candida albicans, Pathogen, 030304 developmental biology

Abstract

Candida aurisis a recently described pathogenic fungus that is causing invasive outbreaks on all continents. The fungus is of high concern given the numbers of multidrug-resistant strains that have been isolated in distinct sites across the globe. The fact that its diagnosis is still problematic suggests that the spreading of the pathogen remains underestimated. Notably, the molecular mechanisms of virulence and antifungal resistance employed by this new species are largely unknown. In the present work, we compared two clinical isolates ofC. auriswith distinct drug susceptibility profiles and aCandida albicansreference strain using a multi-omics approach. Our results show that, despite the distinct drug-resistance profile, bothC. aurisstrains appear to be very similar, albeit with a few notable differences. However, when compared toC. albicansbothC. aurisstrains have major differences regarding their carbon utilization and downstream lipid and protein content, suggesting a multi-factorial mechanism of drug resistance. The molecular profile displayed byC. aurishelps to explain the antifungal resistance and virulence phenotypes of this new emerging pathogen.ImportanceCandida auriswas firstly described in Japan in 2009 and has now been the cause of significant outbreaks across the globe. The high number of isolates that are resistant to one or more antifungals, as well as the high mortality rates from patients with bloodstream infections, has caught the attention of the medical mycology, infectious disease and public health communities to this pathogenic fungus. In the current work, we performed a broad multi-omics approach on two clinical isolates isolated in New York, the most affected area in the USA and found that the omic profile ofC. aurisdiffers significantly fromC. albicans. Besides our insights intoC. auriscarbon utilization and lipid and protein content, we believe that the availability of these data will enhance our ability to combat this rapidly emerging pathogenic yeast.

Published

2019

11. Listeria monocytogenes virulence factors, including listeriolysin O, are secreted in biologically active extracellular vesicles

Author

Maria Maryam, Grégoire Lauvau, Carolina Coelho, Anne Hamacher-Brady, Nathan R. Brady, Raghav Vij, Jennifer E. Kyle, Rafael Prados-Rosales, Daniel F Q Smith, Meagan C. Burnet, Lisa M. Brown, Jasmine Ramirez, Arturo Casadevall, Heino M. Heyman, Ernesto S. Nakayasu, and Isabelle Coppens

Subjects

biology, Listeriolysin O, Virulence, Cell Biology, medicine.disease_cause, biology.organism_classification, Biochemistry, Virulence factor, Microbiology, chemistry.chemical_compound, chemistry, Listeria monocytogenes, Membrane Biology, medicine, Secretion, Peptidoglycan, Bacterial outer membrane, Molecular Biology, Bacteria

Abstract

Outer membrane vesicles produced by Gram-negative bacteria have been studied for half a century but the possibility that Gram-positive bacteria secrete extracellular vesicles (EVs) was not pursued until recently due to the assumption that the thick peptidoglycan cell wall would prevent their release to the environment. However, following their discovery in fungi, which also have cell walls, EVs have now been described for a variety of Gram-positive bacteria. EVs purified from Gram-positive bacteria are implicated in virulence, toxin release, and transference to host cells, eliciting immune responses, and spread of antibiotic resistance. Listeria monocytogenes is a Gram-positive bacterium that causes listeriosis. Here we report that L. monocytogenes produces EVs with diameters ranging from 20 to 200 nm, containing the pore-forming toxin listeriolysin O (LLO) and phosphatidylinositol-specific phospholipase C (PI-PLC). Cell-free EV preparations were toxic to mammalian cells, the murine macrophage cell line J774.16, in a LLO-dependent manner, evidencing EV biological activity. The deletion of plcA increased EV toxicity, suggesting PI-PLC reduced LLO activity. Using simultaneous metabolite, protein, and lipid extraction (MPLEx) multiomics we characterized protein, lipid, and metabolite composition of bacterial cells and secreted EVs and found that EVs carry the majority of listerial virulence proteins. Using immunogold EM we detected LLO at several organelles within infected human epithelial cells and with high-resolution fluorescence imaging we show that dynamic lipid structures are released from L. monocytogenes during infection. Our findings demonstrate that L. monocytogenes uses EVs for toxin release and implicate these structures in mammalian cytotoxicity.

Published

2018

12. Blocking hexose entry into glycolysis activates alternative metabolic conversion of these sugars and upregulates pentose metabolism in Aspergillus nidulans

Author

Khosravi, Claire, Battaglia, Evy, Kun, Roland S., Dalhuijsen, Sacha, Visser, Jaap, Aguilar-Pontes, María Victoria, Zhou, Miaomiao, Heyman, Heino M., Kim, Young Mo, Baker, Scott E., de Vries, Ronald P., Sub Molecular Microbiology, Sub Molecular Plant Physiology, Molecular Plant Physiology, Westerdijk Fungal Biodiversity Institute, Westerdijk Fungal Biodiversity Institute - Fungal Physiology, Sub Molecular Microbiology, Sub Molecular Plant Physiology, and Molecular Plant Physiology

Subjects

0301 basic medicine, lcsh:QH426-470, lcsh:Biotechnology, 030106 microbiology, Pentoses, Pentose, Pentose phosphate pathway, Aspergillus nidulans, Fungal Proteins, 03 medical and health sciences, chemistry.chemical_compound, Gene Expression Regulation, Fungal, Hexokinase, lcsh:TP248.13-248.65, Glucokinase, Genetics, Metabolomics, Glycolysis, Hexose, Hexoses, chemistry.chemical_classification, biology, Catabolism, Central carbon catabolism, Research, Plant biomass degradation, food and beverages, biology.organism_classification, lcsh:Genetics, 030104 developmental biology, chemistry, Biochemistry, Pentose catabolic pathway, Biotechnology

Abstract

Background Plant biomass is the most abundant carbon source for many fungal species. In the biobased industry fungi, are used to produce lignocellulolytic enzymes to degrade agricultural waste biomass. Here we evaluated if it would be possible to create an Aspergillus nidulans strain that releases, but does not metabolize hexoses from plant biomass. For this purpose, metabolic mutants were generated that were impaired in glycolysis, by using hexokinase (hxkA) and glucokinase (glkA) negative strains. To prevent repression of enzyme production due to the hexose accumulation, strains were generated that combined these mutations with a deletion in creA, the repressor involved in regulating preferential use of different carbon catabolic pathways. Results Phenotypic analysis revealed reduced growth for the hxkA1 glkA4 mutant on wheat bran. However, hexoses did not accumulate during growth of the mutants on wheat bran, suggesting that glucose metabolism is re-routed towards alternative carbon catabolic pathways. The creAΔ4 mutation in combination with preventing initial phosphorylation in glycolysis resulted in better growth than the hxkA/glkA mutant and an increased expression of pentose catabolic and pentose phosphate pathway genes. This indicates that the reduced ability to use hexoses as carbon sources created a shift towards the pentose fraction of wheat bran as a major carbon source to support growth. Conclusion Blocking the direct entry of hexoses to glycolysis activates alternative metabolic conversion of these sugars in A. nidulans during growth on plant biomass, but also upregulates conversion of other sugars, such as pentoses. Electronic supplementary material The online version of this article (10.1186/s12864-018-4609-x) contains supplementary material, which is available to authorized users.

Published

2018

13. Listeria monocytogenes virulence factors are secreted in biologically active Extracellular Vesicles

Author

Carolina Coelho, Raghav Vij, Ernesto S. Nakayasu, Jennifer E. Kyle, Anne Hamacher-Brady, Isabelle Coppens, Rafael Prados-Rosales, Lisa M. Brown, Arturo Casadevall, Meagan C. Burnet, Jasmine Ramirez, Grégoire Lauvau, Nathan R. Brady, Heino M. Heyman, and Maria Maryam

Subjects

2. Zero hunger, 0303 health sciences, biology, 030306 microbiology, Toxin, Listeriolysin O, Virulence, medicine.disease_cause, biology.organism_classification, Virulence factor, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, chemistry, Listeria monocytogenes, 13. Climate action, medicine, Peptidoglycan, Bacterial outer membrane, Bacteria, 030304 developmental biology

Abstract

Outer membrane vesicles produced by Gram-negative bacteria have been studied for half a century but the possibility that Gram-positive bacteria secreted extracellular vesicles (EVs) was not pursued due to the assumption that the thick peptidoglycan cell wall would prevent their release to the environment. However, following discovery in fungi, which also have cell walls, EVs have now been described for a variety of Gram-positive bacteria. EVs purified from Gram-positive bacteriaare implicated in virulence, toxin release and transference to host cells, eliciting immune responses, and spread of antibiotic resistance.Listeria monocytogenesis a Gram-positive bacterium that is the etiological agent of listeriosis. Here we report thatL. monocytogenesproduces EVs with diameter ranging from 20-200 nm, containing the pore-forming toxin listeriolysin O(LLO) and phosphatidylinositol-specific phospholipase C (PI-PLC). Using simultaneousmetabolite,protein, andlipidextraction (MPLEx) multi-omics we characterized protein, lipid and metabolite composition of bacterial cells and secreted EVs and found that EVs carry the majority of listerial virulence proteins. Cell-free EV preparations were toxic to the murine macrophage cell line J774.16, in a LLO-dependent manner, evidencing EV biological activity. The deletion ofplcAincreased EV toxicity, suggesting PI-PLC can restrain LLO activity. Using immunogold electron microscopy we detect LLO localization at several organelles within infected human epithelial cells and with high-resolution fluorescence imaging we show that dynamic lipid structures are released fromL. monocytogenesthat colocalize with LLO during infection. Our findings demonstrate thatL. monocytogenesutilize EVs for toxin release and implicate these structures in mammalian cytotoxicity.

Published

2017

14. Antibacterial activity of South African medicinal plants against methicillin resistantStaphylococcus aureus

Author

Ahmed Hussein, Namrita Lall, J.J.M. Meyer, and Heino M. Heyman

Subjects

Pharmacology, biology, Dodonaea viscosa, Pharmaceutical Science, General Medicine, Withania somnifera, Melianthus comosus, biology.organism_classification, medicine.disease_cause, Methicillin-resistant Staphylococcus aureus, Melianthus major, Microbiology, Complementary and alternative medicine, Zygophyllaceae, Staphylococcus aureus, Drug Discovery, medicine, Molecular Medicine, Medicinal plants

Abstract

The rise of infection caused by ‘superbugs’ is alarming and one of the most problematic resistant bacteria is methicillin-resistant Staphylococcus aureus (MRSA). This bacterium can cause a range of ailments like pneumonia, mastitis, meningitis, urinary tract infection, and post operational infection. Ten medicinal plants were investigated for their efficacy against drug-sensitive and drug-resistant strains of S. aureus. Ethanol extracts of Melianthus comosus Vahl (Melianthaceae), Melianthus major L (Melianthaceae), Dodonaea viscosa Jacq. var. angustifolia (L.f.) Benth (Sapindaceae) and Withania somnifera L. Dunal (Zygophyllaceae) were found to have good inhibitory activity against both drug-sensitive and drug-resistant strains of S. aureus. Minimum inhibitory concentrations of these plants ranged from 0.391 to 1.56 mg/ml. Ethanol extracts of all these plants were further tested for cytotoxicity on Vero cells using the XTT method. M. major exhibited a 50% inhibitory concentration (IC50) of 52.76 μg/ml and ...

Published

2009

15. Identification of anti-HIV active dicaffeoylquinic- and tricaffeoylquinic acids in Helichrysum populifolium by NMR-based metabolomic guided fractionation

Author

Isabell Seibert, Heino M. Heyman, François Senejoux, J.J.M. Meyer, Vinesh Maharaj, and Thomas Klimkait

Subjects

Magnetic Resonance Spectroscopy, Anti-HIV Agents, Fractionation, Biology, Chemical Fractionation, chemistry.chemical_compound, Metabolomics, Helichrysum populifolium, Chlorogenic acid, Drug Discovery, Humans, IC50, Pharmacology, Helichrysum, Molecular Structure, Plant Extracts, HIV, General Medicine, Asteraceae, biology.organism_classification, HEK293 Cells, Biochemistry, chemistry, Toxicity, Chlorogenic Acid, HeLa Cells

Abstract

South Africa being home to more than 35% of the world's Helichrysum species (c.a. 244) of which many are used in traditional medicine, is seen potentially as a significant resource in the search of new anti-HIV chemical entities. It was established that five of the 30 Helichrysum species selected for this study had significant anti-HIV activity ranging between 12 and 21 μg/mL (IC50) by using an in-house developed DeCIPhR method on a full virus model. Subsequent toxicity tests also revealed little or no toxicity for these active extracts. With the use of NMR-based metabolomics, the search for common chemical characteristics within the plant extract was conducted, which resulted in specific chemical shift areas identified that could be linked to the anti-HIV activity of the extracts. The NMR chemical shifts associated with the activity were identified to be 2.56-3.08 ppm, 5.24-6.28 ppm, 6.44-7.04 ppm and 7.24-8.04 ppm. This activity profile was then used to guide the fractionation process by narrowing down and focusing the fractionation and purification processes to speed up the putative identification of five compounds with anti-HIV activity in the most active species, Helichrysum populifolium. The anti-HIV compounds identified for the first time from H. populifolium were three dicaffeoylquinic acid derivatives, i.e. 3,4-dicaffeoylquinic acid, 3,5-dicaffeoylquinic acid and 4,5-dicaffeoylquinic acid as well as two tricaffeoylquinic acid derivatives i.e. 1,3,5-tricaffeoylquinic acid and either 5-malonyl-1,3,4-tricaffeoylquinic or 3-malonyl-1,4,5-tricaffeoylquinic acid, with the latter being identified for the first time in the genus.

Published

2015

16. The chemical ‘footprints’ of Euphorbia species found in the mysterious fairy circles of Namibia

Author

Heino M. Heyman, François Senejoux, J.J.M. Meyer, D. Nxumalo, N. Labuschagne, P. Degashu, and N. Galt

Subjects

Euphorbia, biology, Ecology, Botany, Plant Science, biology.organism_classification

Published

2017

17. The only African wild tobacco, Nicotiana africana: alkaloid content and the effect of herbivory

Author

Danica Marlin, Kerstin Krüger, Abdullahi Ahmed Yusuf, Philip C. Stevenson, Susan W. Nicolson, and Heino M. Heyman

Subjects

Nornicotine, Types of tobacco, Nicotine, lcsh:Medicine, Flowers, Helicoverpa armigera, Moths, Anabasine, chemistry.chemical_compound, Alkaloids, Pollinator, Plant-Animal Interactions, Botany, Tobacco, Nectar, Animals, Herbivory, Pollination, lcsh:Science, SB, Flowering Plants, Nicotiana, Multidisciplinary, Chemical Ecology, biology, Ecology, Plant Ecology, fungi, lcsh:R, Organisms, Biology and Life Sciences, Plant-Herbivore Interactions, food and beverages, Plants, biology.organism_classification, Nicotiana africana, Trophic Interactions, Plant Leaves, chemistry, Community Ecology, Plant-Insect Interactions, Larva, Africa, lcsh:Q, Research Article

Abstract

Herbivory in some Nicotiana species is known to induce alkaloid production. This study examined herbivore-induced defenses in the nornicotine-rich African tobacco N. africana, the only Nicotiana species indigenous to Africa. We tested the predictions that: 1) N. africana will have high constitutive levels of leaf, flower and nectar alkaloids; 2) leaf herbivory by the African bollworm Helicoverpa armigera will induce increased alkaloid levels in leaves, flowers and nectar; and 3) increased alkaloid concentrations in herbivore-damaged plants will negatively affect larval growth. We grew N. africana in large pots in a greenhouse and exposed flowering plants to densities of one, three and six fourth-instar larvae of H. armigera, for four days. Leaves, flowers and nectar were analyzed for nicotine, nornicotine and anabasine. The principal leaf alkaloid was nornicotine (mean: 28 µg/g dry mass) followed by anabasine (4.9 µg/g) and nicotine (0.6 µg/g). Nornicotine was found in low quantities in the flowers, but no nicotine or anabasine were recorded. The nectar contained none of the alkaloids measured. Larval growth was reduced when leaves of flowering plants were exposed to six larvae. As predicted by the optimal defense theory, herbivory had a localized effect and caused an increase in nornicotine concentrations in both undamaged top leaves of herbivore damaged plants and herbivore damaged leaves exposed to one and three larvae. The nicotine concentration increased in damaged compared to undamaged middle leaves. The nornicotine concentration was lower in damaged leaves of plants exposed to six compared to three larvae, suggesting that N. africana rather invests in new growth as opposed to protecting older leaves under severe attack. The results indicate that the nornicotine-rich N. africana will be unattractive to herbivores and more so when damaged, but that potential pollinators will be unaffected because the nectar remains alkaloid-free even after herbivory.

Published

2014