Your search keyword '"Michalski WP"' showing total 91 results

1. Cell-mediated and serology-based tests for Mycobacterium ulcerans disease: A systematic review and meta-analysis

Author

Franco-Paredes, C, Avumegah, MS, Waidyatillake, NT, Michalski, WP, O'Brien, DP, Nelson, TM, Athan, E, Franco-Paredes, C, Avumegah, MS, Waidyatillake, NT, Michalski, WP, O'Brien, DP, Nelson, TM, and Athan, E

Abstract

Buruli ulcer (BU) is a subcutaneous necrotic infection of the skin caused by Mycobacterium ulcerans. It is the third most common human mycobacterial disease after tuberculosis (TB) and leprosy. The available methods for detection of the bacilli in lesions are microscopic detection, isolation and cultivation of the bacterium, histopathology, and polymerase chain reaction (PCR). These methods, although approved by the World Health Organization (WHO), have infrastructural and resource challenges in medical centres and cell-mediated immunity (CMI) and/or serology-based tests have been suggested as easier and more appropriate for accurate assessment of the disease, especially in remote or underdeveloped areas. This study systematically reviewed and conducted a meta-analysis for all research aimed at developing cell-mediated immunity (CMI) and/or serology-based tests for M. ulcerans disease. Information for this review was searched through PubMed and Web of Science databases and identified up to June 2019. References from relevant articles and reports from the WHO Annual Meeting of the Global Buruli Ulcer Initiative were also used. Twelve studies beginning in 1952, that attempted to develop CMI and/or serology-based tests for the disease were identified. These studies addressed issues of specificity and sensitivity in context of antigen composition as well as study heterogeneity and bias. The two main types of antigenic preparations considered were pathogen-derived and recombinant protein preparations. There was slight difference in test performance when M. ulcerans recombinant proteins [positivity: 67.5%; 32.5%] or pathogen-derived [positivity: 76.0%; 24.0%] preparations were used as test antigens among BU patients. However, pathogen-derived preparations were better at differentiating between patients and control groups [odds ratio (OR) of 27.92, 95%CI: 5.05-154.28]. This was followed by tests with the recombinant proteins [OR = 1.23, 95%CI: 0.27-5.62]. Overall, study he

Published

2020

2. Pilchard orthomyxovirus (POMV). I. Characterisation of an emerging virus isolated from pilchards Sardinops sagax and Atlantic salmon Salmo salar

Author

Mohr, PG, primary, Crane, MStJ, additional, Hoad, J, additional, Williams, LM, additional, Cummins, D, additional, Neave, MJ, additional, Shiell, B, additional, Beddome, G, additional, Michalski, WP, additional, Peck, GR, additional, Samsing, F, additional, Wynne, JW, additional, Crameri, SG, additional, Hyatt, AD, additional, and Moody, NJG, additional

Published

2020

3. Low incidence of recurrent Buruli ulcers in treated Australian patients living in an endemic region

Author

Pluschke, G, Wynne, JW, Stinear, TP, Athan, E, Michalski, WP, O'Brien, DP, Pluschke, G, Wynne, JW, Stinear, TP, Athan, E, Michalski, WP, and O'Brien, DP

Abstract

We examined recurrent Buruli ulcer cases following treatment and assumed cure in a large cohort of Australian patients living in an endemic area. We report that while the recurrence rate was low (2.81 cases/year/1000 population), it remained similar to the estimated risk of primary infection within the general population of the endemic area (0.85-4.04 cases/year/1,000 population). The majority of recurrent lesions occurred in different regions of the body and were separated by a median time interval of 44 months. Clinical, treatment and epidemiological factors combined with whole genome sequencing of primary and recurrent isolates suggests that in most recurrent cases a re-infection was more likely as opposed to a relapse of the initial infection. Additionally, all cases occurring more than 12 months after commencement of treatment were likely re-infections. Our study provides important prognostic information for patients and their health care providers concerning the nature and risks associated with recurrent cases of Buruli ulcer in Australia.

Published

2018

4. Evolution of high pathogenicity of H5 avian influenza virus: haemagglutinin cleavage site selection of reverse-genetics mutants during passage in chickens

Author

Luczo, JM, Tachedjian, M, Harper, JA, Payne, JS, Butler, JM, Sapats, SI, Lowther, SL, Michalski, WP, Stambas, J, Bingham, J, Luczo, JM, Tachedjian, M, Harper, JA, Payne, JS, Butler, JM, Sapats, SI, Lowther, SL, Michalski, WP, Stambas, J, and Bingham, J

Abstract

Low pathogenicity avian influenza viruses (LPAIVs) are generally asymptomatic in their natural avian hosts. LPAIVs can evolve into highly pathogenic forms, which can affect avian and human populations with devastating consequences. The switch to highly pathogenic avian influenza virus (HPAIV) from LPAIV precursors requires the acquisition of multiple basic amino acids in the haemagglutinin cleavage site (HACS) motif. Through reverse genetics of an H5N1 HPAIV, and experimental infection of chickens, we determined that viruses containing five or more basic amino acids in the HACS motif were preferentially selected over those with three to four basic amino acids, leading to rapid replacement with virus types containing extended HACS motifs. Conversely, viruses harbouring low pathogenicity motifs containing two basic amino acids did not readily evolve to extended forms, suggesting that a single insertion of a basic amino acid into the cleavage site motif of low-pathogenic viruses may lead to escalating selection for extended motifs. Our results may explain why mid-length forms are rarely detected in nature. The stability of the short motif suggests that pathogenicity switching may require specific conditions of intense selection pressure (such as with high host density) to boost selection of the initial mid-length HACS forms.

Published

2018

5. Exposure Risk for Infection and Lack of Human-to-Human Transmission of Mycobacterium ulcerans Disease, Australia

Author

O'Brien, DP, Wynne, JW, Buultjens, AH, Michalski, WP, Stinear, TR, Friedman, ND, Hughes, A, Athan, E, O'Brien, DP, Wynne, JW, Buultjens, AH, Michalski, WP, Stinear, TR, Friedman, ND, Hughes, A, and Athan, E

Abstract

We conducted epidemiologic and genetic analyses of family clusters of Mycobacterium ulcerans (Buruli ulcer) disease in southeastern Australia. We found that the incidence of M. ulcerans disease in family members was increased. However, the risk for exposure appeared short-term and not related to human-human transmission.

Published

2017

6. Proteomics informed by transcriptomics for characterising differential cellular susceptibility to Nelson Bay orthoreovirus infection

Author

Mok, L, Wynne, JW, Tachedjian, M, Shiell, B, Ford, K, Matthews, DA, Bacic, A, Michalski, WP, Mok, L, Wynne, JW, Tachedjian, M, Shiell, B, Ford, K, Matthews, DA, Bacic, A, and Michalski, WP

Abstract

BACKGROUND: Nelson Bay orthoreovirus (NBV) is a fusogenic bat borne virus with an unknown zoonotic potential. Previous studies have shown that NBV can infect and replicate in a wide variety of cell types derived from their natural host (bat), as well as from human, mouse and monkey. Within permissive cells, NBV induced significant cytopathic effects characterised by cell-cell fusion and syncytia formation. To understand the molecular events that underpin NBV infection we examined the host transcriptome and proteome response of two cell types, derived from bat (PaKiT03) and mouse (L929), to characterise differential cellular susceptibility to NBV. RESULTS: Despite significant differences in NBV replication and cytopathic effects in the L929 and PaKiT03 cells, the host response was remarkably similar in these cells. At both the transcriptome and proteome level, the host response was dominated by IFN production and signalling pathways. The majority of proteins up-regulated in L929 and PaKiT03 cells were also up-regulated at the mRNA (gene) level, and included many important IFN stimulated genes. Further functional experimentation demonstrated that stimulating IFN signalling prior to infection, significantly reduced NBV replication in PaKiT03 cells. Moreover, inhibiting IFN signalling (through specific siRNAs) increased NBV replication in L929 cells. In line with the significant cytopathic effects seen in PaKiT03 cells, we also observed a down-regulation of genes involved in cell-cell junctions, which may be related to the fusogenic effects of NBV. CONCLUSIONS: This study provides new multi-dimensional insights into the host response of mammalian cells to NBV infection. We show that IFN activity is capable of reducing NBV replication, although it is unlikely that this is solely responsible for the reduced replication of NBV in L929 cells. The molecular events that underpin the fusogenic cytopathic effects described here will prove valuable for identifying potential ther

Published

2017

7. Dual‐role FilmArray® diagnostics for high‐impact viral diseases

Author

Dorsch, M, primary, Meehan, B, additional, Michalski, WP, additional, Heine, HG, additional, Foord, AJ, additional, Carlile, G, additional, Wang, J, additional, McCullough, S, additional, and Zuelke, K, additional

Published

2016

8. Proteomic analysis of Pteropus alecto kidney cells in response to the viral mimic, Poly I:C

Author

Mok, L, Wynne, JW, Ford, K, Shiell, B, Bacic, A, Michalski, WP, Mok, L, Wynne, JW, Ford, K, Shiell, B, Bacic, A, and Michalski, WP

Abstract

BACKGROUND: Bats are recognised as an important reservoir for a number of highly pathogenic zoonotic viruses. While many of these viruses cause severe and often fatal disease in humans, bats are able to coexist with these viruses without clinical signs of disease. The mechanism conferring this antiviral response is not fully understood. Here, we investigated the differential protein expression of immortalised Pteropus alecto kidney cells (PaKiT03) following transfection with the viral mimic, Poly I:C. Two complementary proteomic approaches, difference gel electrophoresis (DIGE) and isobaric tagging for relative and absolute quantitation (iTRAQ) were used to quantify changes in protein expression following Poly I:C stimulation at 4, 8 and 20 hr post treatment (hpt). RESULTS: The expression of ISG54 gene, a known responder to virus infection and Poly I:C treatment, was significantly induced in transfected cells compared with mock-transfected cells. Through iTRAQ analysis we show that Poly I:C up-regulates key glycolytic enzymes at 4 hpt within PaKiT03 cells. In contrast, at 20 hpt PaKiT03 cells down-regulated ribosomal subunit proteins. The analysis with DIGE of Poly I:C transfected PaKiT03 cells showed over 215 individual spots differentially regulated, however only 25 spots could be unambiguously identified by LC-MS/MS. Immunoblotting confirmed the up-regulation of Eno1 and Tpi1 in PaKiT03 cells following Poly I:C transfection. A comparison with human cells (HEK293T and HeLa) and one additional bat cell line (PaLuT02), demonstrated that glycolytic pathways are also induced in these cell types, but at different intensities. CONCLUSION: The two techniques, DIGE and iTRAQ identified largely overlapping sets of differentially expressed proteins, however DIGE unambiguously identified significantly less proteins than iTRAQ. Poly I:C induced a rapid metabolic shift towards glycolysis within the PaKiT03 cells at 4 hpt, presumably as a consequence of increased energy require

Published

2015

9. Molecular pathogenesis of H5 highly pathogenic avian influenza: the role of the haemagglutinin cleavage site motif

Author

Luczo, JM, Stambas, J, Durr, PA, Michalski, WP, Bingham, J, Luczo, JM, Stambas, J, Durr, PA, Michalski, WP, and Bingham, J

Abstract

The emergence of H5N1 highly pathogenic avian influenza has caused a heavy socio-economic burden through culling of poultry to minimise human and livestock infection. Although human infections with H5N1 have to date been limited, concerns for the pandemic potential of this zoonotic virus have been greatly intensified following experimental evidence of aerosol transmission of H5N1 viruses in a mammalian infection model. In this review, we discuss the dominance of the haemagglutinin cleavage site motif as a pathogenicity determinant, the host-pathogen molecular interactions driving cleavage activation, reverse genetics manipulations and identification of residues key to haemagglutinin cleavage site functionality and the mechanisms of cell and tissue damage during H5N1 infection. We specifically focus on the disease in chickens, as it is in this species that high pathogenicity frequently evolves and from which transmission to the human population occurs. With >75% of emerging infectious diseases being of zoonotic origin, it is necessary to understand pathogenesis in the primary host to explain spillover events into the human population.

Published

2015

10. Exploring the Zoonotic Potential of Mycobacterium avium Subspecies paratuberculosis through Comparative Genomics

Author

Agrewala, JN, Wynne, JW, Bull, TJ, Seemann, T, Bulach, DM, Wagner, J, Kirkwood, CD, Michalski, WP, Agrewala, JN, Wynne, JW, Bull, TJ, Seemann, T, Bulach, DM, Wagner, J, Kirkwood, CD, and Michalski, WP

Abstract

A comparative genomics approach was utilised to compare the genomes of Mycobacterium avium subspecies paratuberculosis (MAP) isolated from early onset paediatric Crohn's disease (CD) patients as well as Johne's diseased animals. Draft genome sequences were produced for MAP isolates derived from four CD patients, one ulcerative colitis (UC) patient, and two non-inflammatory bowel disease (IBD) control individuals using Illumina sequencing, complemented by comparative genome hybridisation (CGH). MAP isolates derived from two bovine and one ovine host were also subjected to whole genome sequencing and CGH. All seven human derived MAP isolates were highly genetically similar and clustered together with one bovine type isolate following phylogenetic analysis. Three other sequenced isolates (including the reference bovine derived isolate K10) were genetically distinct. The human isolates contained two large tandem duplications, the organisations of which were confirmed by PCR. Designated vGI-17 and vGI-18 these duplications spanned 63 and 109 open reading frames, respectively. PCR screening of over 30 additional MAP isolates (3 human derived, 27 animal derived and one environmental isolate) confirmed that vGI-17 and vGI-18 are common across many isolates. Quantitative real-time PCR of vGI-17 demonstrated that the proportion of cells containing the vGI-17 duplication varied between 0.01 to 15% amongst isolates with human isolates containing a higher proportion of vGI-17 compared to most animal isolates. These findings suggest these duplications are transient genomic rearrangements. We hypothesise that the over-representation of vGI-17 in human derived MAP strains may enhance their ability to infect or persist within a human host by increasing genome redundancy and conferring crude regulation of protein expression across biologically important regions.

Published

2011

11. Establishment, Immortalisation and Characterisation of Pteropid Bat Cell Lines

Author

Bereswill, S, Crameri, G, Todd, S, Grimley, S, McEachern, JA, Marsh, GA, Smith, C, Tachedjian, M, De Jong, C, Virtue, ER, Yu, M, Bulach, D, Liu, J-P, Michalski, WP, Middleton, D, Field, HE, Wang, L-F, Bereswill, S, Crameri, G, Todd, S, Grimley, S, McEachern, JA, Marsh, GA, Smith, C, Tachedjian, M, De Jong, C, Virtue, ER, Yu, M, Bulach, D, Liu, J-P, Michalski, WP, Middleton, D, Field, HE, and Wang, L-F

Abstract

BACKGROUND: Bats are the suspected natural reservoir hosts for a number of new and emerging zoonotic viruses including Nipah virus, Hendra virus, severe acute respiratory syndrome coronavirus and Ebola virus. Since the discovery of SARS-like coronaviruses in Chinese horseshoe bats, attempts to isolate a SL-CoV from bats have failed and attempts to isolate other bat-borne viruses in various mammalian cell lines have been similarly unsuccessful. New stable bat cell lines are needed to help with these investigations and as tools to assist in the study of bat immunology and virus-host interactions. METHODOLOGY/FINDINGS: Black flying foxes (Pteropus alecto) were captured from the wild and transported live to the laboratory for primary cell culture preparation using a variety of different methods and culture media. Primary cells were successfully cultured from 20 different organs. Cell immortalisation can occur spontaneously, however we used a retroviral system to immortalise cells via the transfer and stable production of the Simian virus 40 Large T antigen and the human telomerase reverse transcriptase protein. Initial infection experiments with both cloned and uncloned cell lines using Hendra and Nipah viruses demonstrated varying degrees of infection efficiency between the different cell lines, although it was possible to infect cells in all tissue types. CONCLUSIONS/SIGNIFICANCE: The approaches developed and optimised in this study should be applicable to bats of other species. We are in the process of generating further cell lines from a number of different bat species using the methodology established in this study.

Published

2009

12. Detection and measurement of carbohydrate deficient transferrin in serum using immuno-capture mass spectrometry: Diagnostic applications for annual ryegrass toxicity and corynetoxin exposure

Author

Megan A. S. Penno, Wojtek P. Michalski, Steven M. Colegate, Peter Hoffmann, Penno, MAS, Colegate, SM, Michalski, WP, and Hoffmann, P

Subjects

MALDI-TOF, mass spectrometry profiling, Carbohydrates, Carbohydrate deficient transferrin, Enzyme-Linked Immunosorbent Assay, Mass spectrometry, Proteomics, Sensitivity and Specificity, Microbiology, proteomics, Glycolipid, Lolium, Animals, Disease biomarker, Ingestion, Veterinary Sciences, Ryegrass toxicity, Toxicity Tests, Chronic, chemistry.chemical_classification, annual ryegrass toxicity, Chromatography, General Veterinary, Transferrin, biomarkers, Reproducibility of Results, Rats, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Glycolipids, Biomarkers

Abstract

The neurological livestock disease annual ryegrass toxicity (ARGT) is caused by the ingestion of the naturally occurring glycolipid toxins - the corynetoxins. Corynetoxins also threaten human health as potential contaminants of the food supply. Presently, there are no routine diagnostic tests for corynetoxins-exposure in humans or livestock. Chronic ingestion of corynetoxins has been modeled in rats exposed to dietary tunicamycins for 12 months and carbohydrate deficient transferrin (CDT) has been previously identified as a candidate disease biomarker. Here, the technique of immuno-capture mass spectrometry (icMS) was used to evaluate serum levels of CDT, discriminating between control and tunicamycins-exposed rats with 85% accuracy. The icMS approach is based on the combination of specific transferrin enrichment with functionalized magnetic beads and automated matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS). With no other clinically-relevant diagnostic tests available icMS could be readily adapted for high-throughput clinical assessment of corynetoxins-exposure in humans or livestock. Refereed/Peer-reviewed

Published

2012

13. Reagents for detection of Rift Valley fever virus infection in sheep.

Author

Shiell BJ, Ye S, Harper JA, van der Heide B, Beddome G, Foord AJ, Michalski WP, Bingham J, and Peck GR

Subjects

Animals, Indicators and Reagents chemistry, Sheep, Rift Valley Fever diagnosis, Rift Valley fever virus isolation & purification, Sheep Diseases diagnosis

Abstract

Rift Valley fever virus (RVFV) causes Rift Valley fever (RVF), resulting in morbidity and mortality in humans and ruminants. Evidence of transboundary outbreaks means that RVFV remains a threat to human health and livestock industries in countries that are free from the disease. To enhance surveillance capability, methods for detection of RVFV are required. The generation of reagents suitable for the detection of RVFV antigen in formalin-fixed, paraffin-embedded tissues from infected animals have been developed and are described herein. Recombinant nucleoprotein (rNP) was expressed in Escherichia coli and purified using immobilized metal ion affinity chromatography. Purified rNP was used as an immunogen to produce anti-NP polyclonal antisera in rabbits for use in detection of RVFV NP in experimentally infected animals by immunohistochemistry. Antisera raised in rabbits against rNP were able to recognize viral NP antigen in fixed infected Vero cell pellets and sheep liver. Therefore, the methods and reagents described herein are useful in assays for detection of RVFV infections in animals, for research and surveillance purposes.

Published

2020

14. Cell-mediated and serology-based tests for Mycobacterium ulcerans disease: A systematic review and meta-analysis.

Author

Avumegah MS, Waidyatillake NT, Michalski WP, O'Brien DP, Nelson TM, and Athan E

Subjects

Buruli Ulcer microbiology, Buruli Ulcer pathology, Databases, Factual, Humans, Immunity, Cellular, Leprosy, Polymerase Chain Reaction, Buruli Ulcer diagnosis, Mycobacterium ulcerans isolation & purification, Serologic Tests methods

Abstract

Buruli ulcer (BU) is a subcutaneous necrotic infection of the skin caused by Mycobacterium ulcerans. It is the third most common human mycobacterial disease after tuberculosis (TB) and leprosy. The available methods for detection of the bacilli in lesions are microscopic detection, isolation and cultivation of the bacterium, histopathology, and polymerase chain reaction (PCR). These methods, although approved by the World Health Organization (WHO), have infrastructural and resource challenges in medical centres and cell-mediated immunity (CMI) and/or serology-based tests have been suggested as easier and more appropriate for accurate assessment of the disease, especially in remote or underdeveloped areas. This study systematically reviewed and conducted a meta-analysis for all research aimed at developing cell-mediated immunity (CMI) and/or serology-based tests for M. ulcerans disease. Information for this review was searched through PubMed and Web of Science databases and identified up to June 2019. References from relevant articles and reports from the WHO Annual Meeting of the Global Buruli Ulcer Initiative were also used. Twelve studies beginning in 1952, that attempted to develop CMI and/or serology-based tests for the disease were identified. These studies addressed issues of specificity and sensitivity in context of antigen composition as well as study heterogeneity and bias. The two main types of antigenic preparations considered were pathogen-derived and recombinant protein preparations. There was slight difference in test performance when M. ulcerans recombinant proteins [positivity: 67.5%; 32.5%] or pathogen-derived [positivity: 76.0%; 24.0%] preparations were used as test antigens among BU patients. However, pathogen-derived preparations were better at differentiating between patients and control groups [odds ratio (OR) of 27.92, 95%CI: 5.05-154.28]. This was followed by tests with the recombinant proteins [OR = 1.23, 95%CI: 0.27-5.62]. Overall, study heterogeneity index, I2 was 92.4% (p = 0.000). It is apparent from this review that standardisation is needed in any future CMI and/or serology-based tests used for M. ulcerans disease., Competing Interests: The authors have declared that no competing interests exist.

Published

2020

15. Low incidence of recurrent Buruli ulcers in treated Australian patients living in an endemic region.

Author

Wynne JW, Stinear TP, Athan E, Michalski WP, and O'Brien DP

Subjects

Adult, Aged, Aged, 80 and over, Australia, Buruli Ulcer drug therapy, Buruli Ulcer microbiology, Buruli Ulcer pathology, Cohort Studies, Female, Humans, Male, Middle Aged, Phylogeny, Recurrence, Risk Factors, Time Factors, Young Adult, Anti-Bacterial Agents therapeutic use, Buruli Ulcer epidemiology, Mycobacterium ulcerans genetics

Abstract

We examined recurrent Buruli ulcer cases following treatment and assumed cure in a large cohort of Australian patients living in an endemic area. We report that while the recurrence rate was low (2.81 cases/year/1000 population), it remained similar to the estimated risk of primary infection within the general population of the endemic area (0.85-4.04 cases/year/1,000 population). The majority of recurrent lesions occurred in different regions of the body and were separated by a median time interval of 44 months. Clinical, treatment and epidemiological factors combined with whole genome sequencing of primary and recurrent isolates suggests that in most recurrent cases a re-infection was more likely as opposed to a relapse of the initial infection. Additionally, all cases occurring more than 12 months after commencement of treatment were likely re-infections. Our study provides important prognostic information for patients and their health care providers concerning the nature and risks associated with recurrent cases of Buruli ulcer in Australia., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

16. Evolution of high pathogenicity of H5 avian influenza virus: haemagglutinin cleavage site selection of reverse-genetics mutants during passage in chickens.

Author

Luczo JM, Tachedjian M, Harper JA, Payne JS, Butler JM, Sapats SI, Lowther SL, Michalski WP, Stambas J, and Bingham J

Subjects

Animals, Chickens, Influenza A Virus, H5N1 Subtype genetics, Influenza A Virus, H5N1 Subtype isolation & purification, Influenza in Birds virology, Poultry Diseases, Proteolysis, Reverse Genetics, Selection, Genetic, Hemagglutinin Glycoproteins, Influenza Virus genetics, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Influenza A Virus, H5N1 Subtype pathogenicity, Mutant Proteins genetics, Mutant Proteins metabolism

Abstract

Low pathogenicity avian influenza viruses (LPAIVs) are generally asymptomatic in their natural avian hosts. LPAIVs can evolve into highly pathogenic forms, which can affect avian and human populations with devastating consequences. The switch to highly pathogenic avian influenza virus (HPAIV) from LPAIV precursors requires the acquisition of multiple basic amino acids in the haemagglutinin cleavage site (HACS) motif. Through reverse genetics of an H5N1 HPAIV, and experimental infection of chickens, we determined that viruses containing five or more basic amino acids in the HACS motif were preferentially selected over those with three to four basic amino acids, leading to rapid replacement with virus types containing extended HACS motifs. Conversely, viruses harbouring low pathogenicity motifs containing two basic amino acids did not readily evolve to extended forms, suggesting that a single insertion of a basic amino acid into the cleavage site motif of low-pathogenic viruses may lead to escalating selection for extended motifs. Our results may explain why mid-length forms are rarely detected in nature. The stability of the short motif suggests that pathogenicity switching may require specific conditions of intense selection pressure (such as with high host density) to boost selection of the initial mid-length HACS forms.

Published

2018

17. Dark-chilling and subsequent photo-activation modulate expression and induce reversible association of chloroplast lipoxygenase with thylakoid membrane in runner bean (Phaseolus coccineus L.).

Author

Mazur R, Trzcinska-Danielewicz J, Kozlowski P, Kowalewska Ł, Rumak I, Shiell BJ, Mostowska A, Michalski WP, and Garstka M

Subjects

Cold Temperature, Light, Lipoxygenase metabolism, Phaseolus enzymology, Plant Proteins metabolism, Thylakoids enzymology

Abstract

Lipoxygenases (LOXs) are non-haem iron-containing dioxygenases that catalyse oxygenation of polyunsaturated fatty acids. This reaction is the first step in biosynthesis of oxylipins, which play important and diverse roles in stress response. In this study, we identified four LOX genes (PcLOXA, B, C, D) in chilling-sensitive runner bean (Phaseolus coccineus L.) plant and analyzed their expression patterns during long term dark-chilling (4 °C) stress and during day/night (21ºC/4 °C) temperature fluctuations. Three of the four identified LOX genes, namely PcLOXA, PcLOXB and PcLOXD, were induced by wounding stress, while only the PcLOXA was induced by dark-chilling of both detached (wounded) leaves and whole plants. We identified PcLOXA as a chloroplast-targeted LOX protein and investigated its expression during chilling stress in terms of abundance, localization inside chloroplasts and interactions with the thylakoid membranes. The analysis by immunogold electron microscopy has shown that more than 60% of detectable PcLOXA protein was associated with thylakoids, and dark-chilling of leaves resulted in increased amounts of this protein detected within grana margins of thylakoids. This effect was reversible under subsequent photo-activation of chilled leaves. PcLOXA binding to thylakoids is not mediated by the posttranslational modification but rather is based on direct interactions of the protein with membrane lipids; the binding strength increases under dark-chilling conditions., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)

Published

2018

18. Development and validation of an immunoperoxidase antigen detection test for improved diagnosis of rabies in Indonesia.

Author

Rahmadane I, Certoma AF, Peck GR, Fitria Y, Payne J, Colling A, Shiell BJ, Beddome G, Wilson S, Yu M, Morrissy C, Michalski WP, Bingham J, Gardner IA, and Allen JD

Subjects

Animals, Brain virology, Gene Expression Regulation, Viral, Humans, Immunization, Immunoenzyme Techniques economics, Indonesia epidemiology, Nucleoproteins immunology, Nucleoproteins isolation & purification, Rabbits, Rabies epidemiology, Reagent Kits, Diagnostic, Reproducibility of Results, Viral Proteins immunology, Viral Proteins isolation & purification, Antigens, Viral, Immunoenzyme Techniques methods, Rabies diagnosis, Rabies virus isolation & purification

Abstract

Rabies continues to pose a significant threat to human and animal health in regions of Indonesia. Indonesia has an extensive network of veterinary diagnostic laboratories and the 8 National laboratories are equipped to undertake diagnostic testing for rabies using the commercially-procured direct fluorescent antibody test (FAT), which is considered the reference (gold standard) test. However, many of the Indonesian Provincial diagnostic laboratories do not have a fluorescence microscope required to undertake the FAT. Instead, certain Provincial laboratories continue to screen samples using a chemical stain-based test (Seller's stain test, SST). This test has low diagnostic sensitivity, with negative SST-tested samples being forwarded to the nearest National laboratory resulting in significant delays for completion of testing and considerable additional costs. This study sought to develop a cost-effective and diagnostically-accurate immunoperoxidase antigen detection (RIAD) test for rabies that can be readily and quickly performed by the resource-constrained Provincial laboratories. This would reduce the burden on the National laboratories and allow more rapid diagnoses and implementation of post-exposure prophylaxis. The RIAD test was evaluated using brain smears fixed with acetone or formalin and its performance was validated by comparison with established rabies diagnostic tests used in Indonesia, including the SST and FAT. A proficiency testing panel was distributed between Provincial laboratories to assess the reproducibility of the test. The performance of the RIAD test was improved by using acetone fixation of brain smears rather than formalin fixation such that it was of equivalent accuracy to that of the World Organisation for Animal Health (OIE)-recommended FAT, with both tests returning median diagnostic sensitivity and specificity values of 0.989 and 0.993, respectively. The RIAD test and FAT had higher diagnostic sensitivity than the SST (median = 0.562). Proficiency testing using a panel of 6 coded samples distributed to 16 laboratories showed that the RIAD test had good reproducibility with an overall agreement of 97%. This study describes the successful development, characterisation and use of a novel RIAD test and its fitness for purpose as a screening test for use in provincial Indonesian veterinary laboratories.

Published

2017

19. Proteomics informed by transcriptomics for characterising differential cellular susceptibility to Nelson Bay orthoreovirus infection.

Author

Mok L, Wynne JW, Tachedjian M, Shiell B, Ford K, Matthews DA, Bacic A, and Michalski WP

Subjects

Animals, Cell Line, Chiroptera virology, Interferons metabolism, Mice, RNA, Messenger genetics, RNA, Messenger metabolism, Signal Transduction genetics, Virus Replication, Gene Expression Profiling, Orthoreovirus physiology, Proteomics

Abstract

Background: Nelson Bay orthoreovirus (NBV) is a fusogenic bat borne virus with an unknown zoonotic potential. Previous studies have shown that NBV can infect and replicate in a wide variety of cell types derived from their natural host (bat), as well as from human, mouse and monkey. Within permissive cells, NBV induced significant cytopathic effects characterised by cell-cell fusion and syncytia formation. To understand the molecular events that underpin NBV infection we examined the host transcriptome and proteome response of two cell types, derived from bat (PaKiT03) and mouse (L929), to characterise differential cellular susceptibility to NBV., Results: Despite significant differences in NBV replication and cytopathic effects in the L929 and PaKiT03 cells, the host response was remarkably similar in these cells. At both the transcriptome and proteome level, the host response was dominated by IFN production and signalling pathways. The majority of proteins up-regulated in L929 and PaKiT03 cells were also up-regulated at the mRNA (gene) level, and included many important IFN stimulated genes. Further functional experimentation demonstrated that stimulating IFN signalling prior to infection, significantly reduced NBV replication in PaKiT03 cells. Moreover, inhibiting IFN signalling (through specific siRNAs) increased NBV replication in L929 cells. In line with the significant cytopathic effects seen in PaKiT03 cells, we also observed a down-regulation of genes involved in cell-cell junctions, which may be related to the fusogenic effects of NBV., Conclusions: This study provides new multi-dimensional insights into the host response of mammalian cells to NBV infection. We show that IFN activity is capable of reducing NBV replication, although it is unlikely that this is solely responsible for the reduced replication of NBV in L929 cells. The molecular events that underpin the fusogenic cytopathic effects described here will prove valuable for identifying potential therapeutic targets against fusogenic orthoreovirus.

Published

2017

20. Exposure Risk for Infection and Lack of Human-to-Human Transmission of Mycobacterium ulcerans Disease, Australia.

Author

O'Brien DP, Wynne JW, Buultjens AH, Michalski WP, Stinear TP, Friedman ND, Hughes A, and Athan E

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Australia epidemiology, Buruli Ulcer transmission, Child, Child, Preschool, Environmental Exposure, Female, Genome, Viral, Humans, Incidence, Male, Middle Aged, Phylogeny, Polymorphism, Single Nucleotide, Risk, Young Adult, Buruli Ulcer epidemiology, Buruli Ulcer microbiology, Mycobacterium ulcerans classification, Mycobacterium ulcerans genetics, Mycobacterium ulcerans isolation & purification

Abstract

We conducted epidemiologic and genetic analyses of family clusters of Mycobacterium ulcerans (Buruli ulcer) disease in southeastern Australia. We found that the incidence of M. ulcerans disease in family members was increased. However, the risk for exposure appeared short-term and not related to human-human transmission.

Published

2017

21. Contraction of the type I IFN locus and unusual constitutive expression of IFN-α in bats.

Author

Zhou P, Tachedjian M, Wynne JW, Boyd V, Cui J, Smith I, Cowled C, Ng JH, Mok L, Michalski WP, Mendenhall IH, Tachedjian G, Wang LF, and Baker ML

Subjects

Animals, Base Sequence, Cell Line, Chiroptera metabolism, Chiroptera virology, Chromosome Mapping, Evolution, Molecular, HEK293 Cells, Hendra Virus physiology, Host-Pathogen Interactions, Humans, Immunoblotting, Interferon Type I metabolism, Interferon-alpha metabolism, Molecular Sequence Data, Reverse Transcriptase Polymerase Chain Reaction, Sequence Analysis, DNA, Sequence Homology, Nucleic Acid, Chiroptera genetics, Gene Expression Profiling, Interferon Type I genetics, Interferon-alpha genetics

Abstract

Bats harbor many emerging and reemerging viruses, several of which are highly pathogenic in other mammals but cause no clinical signs of disease in bats. To determine the role of interferons (IFNs) in the ability of bats to coexist with viruses, we sequenced the type I IFN locus of the Australian black flying fox, Pteropus alecto, providing what is, to our knowledge, the first gene map of the IFN region of any bat species. Our results reveal a highly contracted type I IFN family consisting of only 10 IFNs, including three functional IFN-α loci. Furthermore, the three IFN-α genes are constitutively expressed in unstimulated bat tissues and cells and their expression is unaffected by viral infection. Constitutively expressed IFN-α results in the induction of a subset of IFN-stimulated genes associated with antiviral activity and resistance to DNA damage, providing evidence for a unique IFN system that may be linked to the ability of bats to coexist with viruses.

Published

2016

22. Proteomic analysis of Pteropus alecto kidney cells in response to the viral mimic, Poly I:C.

Author

Mok L, Wynne JW, Ford K, Shiell B, Bacic A, and Michalski WP

Abstract

Background: Bats are recognised as an important reservoir for a number of highly pathogenic zoonotic viruses. While many of these viruses cause severe and often fatal disease in humans, bats are able to coexist with these viruses without clinical signs of disease. The mechanism conferring this antiviral response is not fully understood. Here, we investigated the differential protein expression of immortalised Pteropus alecto kidney cells (PaKiT03) following transfection with the viral mimic, Poly I:C. Two complementary proteomic approaches, difference gel electrophoresis (DIGE) and isobaric tagging for relative and absolute quantitation (iTRAQ) were used to quantify changes in protein expression following Poly I:C stimulation at 4, 8 and 20 hr post treatment (hpt)., Results: The expression of ISG54 gene, a known responder to virus infection and Poly I:C treatment, was significantly induced in transfected cells compared with mock-transfected cells. Through iTRAQ analysis we show that Poly I:C up-regulates key glycolytic enzymes at 4 hpt within PaKiT03 cells. In contrast, at 20 hpt PaKiT03 cells down-regulated ribosomal subunit proteins. The analysis with DIGE of Poly I:C transfected PaKiT03 cells showed over 215 individual spots differentially regulated, however only 25 spots could be unambiguously identified by LC-MS/MS. Immunoblotting confirmed the up-regulation of Eno1 and Tpi1 in PaKiT03 cells following Poly I:C transfection. A comparison with human cells (HEK293T and HeLa) and one additional bat cell line (PaLuT02), demonstrated that glycolytic pathways are also induced in these cell types, but at different intensities., Conclusion: The two techniques, DIGE and iTRAQ identified largely overlapping sets of differentially expressed proteins, however DIGE unambiguously identified significantly less proteins than iTRAQ. Poly I:C induced a rapid metabolic shift towards glycolysis within the PaKiT03 cells at 4 hpt, presumably as a consequence of increased energy requirements. On the other hand ribosomal subunit proteins were seen as down-regulated by iTRAQ, these proteins may be the limiting factors in the translational machinery available for virus replication. This study provides new insight into the antiviral response of bat cells, highlighting the importance of energy metabolism.

Published

2015

23. Molecular pathogenesis of H5 highly pathogenic avian influenza: the role of the haemagglutinin cleavage site motif.

Author

Luczo JM, Stambas J, Durr PA, Michalski WP, and Bingham J

Subjects

Animals, Chickens, Humans, Influenza in Birds transmission, Zoonoses pathology, Zoonoses transmission, Zoonoses virology, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Host-Pathogen Interactions, Influenza A Virus, H5N1 Subtype pathogenicity, Influenza in Birds pathology, Influenza in Birds virology, Proteolysis, Virulence Factors metabolism

Abstract

The emergence of H5N1 highly pathogenic avian influenza has caused a heavy socio-economic burden through culling of poultry to minimise human and livestock infection. Although human infections with H5N1 have to date been limited, concerns for the pandemic potential of this zoonotic virus have been greatly intensified following experimental evidence of aerosol transmission of H5N1 viruses in a mammalian infection model. In this review, we discuss the dominance of the haemagglutinin cleavage site motif as a pathogenicity determinant, the host-pathogen molecular interactions driving cleavage activation, reverse genetics manipulations and identification of residues key to haemagglutinin cleavage site functionality and the mechanisms of cell and tissue damage during H5N1 infection. We specifically focus on the disease in chickens, as it is in this species that high pathogenicity frequently evolves and from which transmission to the human population occurs. With >75% of emerging infectious diseases being of zoonotic origin, it is necessary to understand pathogenesis in the primary host to explain spillover events into the human population., (© 2015 The Authors. Reviews in Medical Virology published by John Wiley & Sons Ltd.)

Published

2015

24. Mouse fibroblast L929 cells are less permissive to infection by Nelson Bay orthoreovirus compared to other mammalian cell lines.

Author

Mok L, Wynne JW, Grimley S, Shiell B, Green D, Monaghan P, Pallister J, Bacic A, and Michalski WP

Subjects

Animals, Chiroptera, Haplorhini, Humans, Mice, Orthoreovirus growth & development, Viral Load, Virus Cultivation, Virus Replication, Cell Line virology, Fibroblasts virology, Orthoreovirus physiology, Viral Tropism

Abstract

In recent years, bats have been identified as a natural reservoir for a diverse range of viruses. Nelson Bay orthoreovirus (NBV) was first isolated from the heart blood of a fruit bat (Pteropus poliocephalus) in 1968. While the pathogenesis of NBV remains unknown, other related members of this group have caused acute respiratory disease in humans. Thus the potential for NBV to impact human health appears plausible. Here, to increase our knowledge of NBV, we examined the replication and infectivity of NBV using different mammalian cell lines derived from bat, human, mouse and monkey. All cell lines supported the replication of NBV; however, L929 cells showed a greater than 2 log reduction in virus titre compared with the other cell lines. Furthermore, NBV did not induce major cytopathic effects in the L929 cells, as was observed in other cell lines. Interestingly, the related Pteropine orthoreoviruses, Pulau virus (PulV) and Melaka virus (MelV) were able to replicate to high titres in L929 cells but infection resulted in reduced cytopathic effect. Our study demonstrates a unique virus-host interaction between NBV and L929 cells, where cells effectively control viral infection/replication and limit the formation of syncytia. By elucidating the molecular mechanisms that control this unique relationship, important insights will be made into the biology of this fusogenic virus.

Published

2015

25. Pan-Serotype Diagnostic for Foot-and-Mouth Disease Using the Consensus Antigen of Nonstructural Protein 3B.

Author

Van Dreumel AK, Michalski WP, McNabb LM, Shiell BJ, Singanallur NB, and Peck GR

Subjects

Amino Acid Sequence, Animals, Cattle, Enzyme-Linked Immunosorbent Assay, Molecular Sequence Data, Antibodies, Viral blood, Foot-and-Mouth Disease diagnosis, Foot-and-Mouth Disease immunology, Foot-and-Mouth Disease Virus immunology, Viral Nonstructural Proteins immunology

Abstract

An amino acid consensus sequence for the seven serotypes of foot-and-mouth disease virus (FMDV) nonstructural protein 3B, including all three contiguous repeats, and its use in the development of a pan-serotype diagnostic test for all seven FMDV serotypes are described. The amino acid consensus sequence of the 3B protein was determined from a multiple-sequence alignment of 125 sequences of 3B. The consensus 3B (c3B) protein was expressed as a soluble recombinant fusion protein with maltose-binding protein (MBP) using a bacterial expression system and was affinity purified using amylose resin. The MBP-c3B protein was used as the antigen in the development of a competition enzyme-linked immunosorbent assay (cELISA) for detection of anti-3B antibodies in bovine sera. The comparative diagnostic sensitivity and specificity at 47% inhibition were estimated to be 87.22% and 93.15%, respectively. Reactivity of c3B with bovine sera representing the seven FMDV serotypes demonstrated the pan-serotype diagnostic capability of this bioreagent. The consensus antigen and competition ELISA are described here as candidates for a pan-serotype diagnostic test for FMDV infection., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

26. SNP genotyping of animal and human derived isolates of Mycobacterium avium subsp. paratuberculosis.

Author

Wynne JW, Beller C, Boyd V, Francis B, Gwoźdź J, Carajias M, Heine HG, Wagner J, Kirkwood CD, and Michalski WP

Subjects

Animals, Australia, Cattle, Humans, Mycobacterium avium subsp. paratuberculosis isolation & purification, Paratuberculosis epidemiology, Phylogeny, Polymorphism, Single Nucleotide, Sheep genetics, Genotype, Mycobacterium avium subsp. paratuberculosis genetics, Paratuberculosis microbiology

Abstract

Mycobacterium avium subsp. paratuberculosis (MAP) is the aetiological agent of Johne's disease (JD), a chronic granulomatous enteritis that affects ruminants worldwide. While the ability of MAP to cause disease in animals is clear, the role of this bacterium in human inflammatory bowel diseases remains unresolved. Previous whole genome sequencing of MAP isolates derived from human and three animal hosts showed that human isolates were genetically similar and showed a close phylogenetic relationship to one bovine isolate. In contrast, other animal derived isolates were more genetically diverse. The present study aimed to investigate the frequency of this human strain across 52 wild-type MAP isolates, collected predominantly from Australia. A Luminex based SNP genotyping approach was utilised to genotype SNPs that had previously been shown to be specific to the human, bovine or ovine isolate types. Fourteen SNPs were initially evaluated across a reference panel of isolates with known genotypes. A subset of seven SNPs was chosen for analysis within the wild-type collection. Of the seven SNPs, three were found to be unique to paediatric human isolates. No wild-type isolates contain these SNP alleles. Interestingly, and in contrast to the paediatric isolates, three additional adult human isolates (derived from adult Crohn's disease patients) also did not contain these SNP alleles. Furthermore we identified two SNPs, which demonstrate extensive polymorphism within the animal-derived MAP isolates. One of which appears unique to ovine and a single camel isolate. From this study we suggest the existence of genetic heterogeneity between human derived MAP isolates, some of which are highly similar to those derived from bovine hosts, but others of which are more divergent., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2014

27. Increased bacterial cell density and recombinant protein yield using a commercial microbial cultivation system.

Author

Peck GR, Bowden TR, Shiell BJ, and Michalski WP

Subjects

Bioreactors, Cloning, Molecular, Culture Media metabolism, Escherichia coli cytology, Escherichia coli metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Solubility, Viral Proteins chemistry, Viral Proteins metabolism, Capripoxvirus genetics, Escherichia coli genetics, Industrial Microbiology instrumentation, Recombinant Proteins genetics, Viral Proteins genetics

Abstract

EnBase (BioSilta, Finland) is a microbial cultivation system that replicates fed-batch systems through sustained release of glucose by enzymatic degradation of a polymeric substrate. Achievable bacterial cell densities and recombinant capripoxvirus protein expression levels, solubility, and antigenicity using the EnBase system were assessed. BL21-AI Escherichia coli expressing capripoxvirus proteins achieved up to eightfold higher cell densities when grown in EnBase media compared with standard media. Greater yields of capripoxvirus proteins were attained using EnBase media, either through increases in the amount of expressed protein per cell in conjunction with higher cell density or through the increase in cell density alone. Addition of EnBase booster enhanced protein yield for one of the proteins tested but reduced yield for the other. However, the amount of soluble forms of the capripoxvirus proteins tested was not different from that observed from cultures grown under standard conditions. Purified capripoxvirus proteins expressed using EnBase or standard media were assessed for their performance by enzyme-linked immunosorbent assay (ELISA) and were shown to be equally capable of specifically binding capripoxvirus antibodies.

Published

2014

28. TLR4, IL10RA, and NOD2 mutation in paediatric Crohn's disease patients: an association with Mycobacterium avium subspecies paratuberculosis and TLR4 and IL10RA expression.

Author

Wagner J, Skinner NA, Catto-Smith AG, Cameron DJ, Michalski WP, Visvanathan K, and Kirkwood CD

Subjects

Adolescent, Child, Crohn Disease immunology, Female, Gene Expression, Humans, Interleukin-10 Receptor alpha Subunit biosynthesis, Interleukin-10 Receptor alpha Subunit immunology, Male, Mycobacterium avium subsp. paratuberculosis isolation & purification, Nod2 Signaling Adaptor Protein immunology, Toll-Like Receptor 4 biosynthesis, Toll-Like Receptor 4 immunology, Crohn Disease genetics, Genetic Predisposition to Disease, Interleukin-10 Receptor alpha Subunit genetics, Mycobacterium avium subsp. paratuberculosis immunology, Nod2 Signaling Adaptor Protein genetics, Polymorphism, Single Nucleotide, Toll-Like Receptor 4 genetics

Abstract

Mycobacterium avium subspecies paratuberculosis (MAP) has been implicated in the pathogenesis of Crohn's disease (CD). The role of CD susceptibility genes in association with these microbes is not known. Sixty-two early onset paediatric CD patients and 46 controls with known MAP status were analysed for an association with 34 single nucleotide polymorphisms (SNPs) from 18 CD susceptibility genes. Functional studies on peripheral blood mononuclear cells (PBMCs) were conducted on 17 CD patients with known CD mutations to assess IL-6, IL-10, and TNF-α expression upon stimulation with MAP precipitated protein derivative (PPD) and lipopolysaccharide (LPS). In addition, surface expression of IL10R and TLR4 on resting B cells, NK cells, T cells, and monocytes was assessed. A mutation in TLR4 (rs4986790) and IL10RA (rs22291130) was significantly associated with MAP-positive CD patients compared to MAP-negative CD patients (27.6 vs. 6.1 %, p = 0.021, and 62.1 vs. 33.3 %, p = 0.024, respectively). PPD and LPS significantly increased IL-6, IL-10, and TNF-α production in PBMCs. IL-10 and TNF-α production were significantly lower in a subgroup of CD patients (5/12) with a known NOD2 mutation. Receptor for IL-10 was significantly higher expressed on NK cells (CD56low) and on NK T cells harbouring a NOD2 mutations compared to wildtype cells (p = 0.031 and 0.005, respectively). TLR4 was significantly higher expressed on NK cells (CD56high) harbouring a NOD2 mutations compared to wildtype cells (p = 0.038).

Published

2013

29. Purification and characterisation of immunoglobulins from the Australian black flying fox (Pteropus alecto) using anti-fab affinity chromatography reveals the low abundance of IgA.

Author

Wynne JW, Di Rubbo A, Shiell BJ, Beddome G, Cowled C, Peck GR, Huang J, Grimley SL, Baker ML, and Michalski WP

Subjects

Animals, Immunoglobulin A isolation & purification, Immunoglobulins isolation & purification, Chiroptera immunology, Chromatography, Affinity methods, Immunoglobulin A analysis, Immunoglobulins analysis

Abstract

There is now an overwhelming body of evidence that implicates bats in the dissemination of a long list of emerging and re-emerging viral agents, often causing illnesses or death in both animals and humans. Despite this, there is a paucity of information regarding the immunological mechanisms by which bats coexist with highly pathogenic viruses. Immunoglobulins are major components of the adaptive immune system. Early studies found bats may have quantitatively lower antibody responses to model antigens compared to conventional laboratory animals. To further understand the antibody response of bats, the present study purified and characterised the major immunoglobulin classes from healthy black flying foxes, Pteropus alecto. We employed a novel strategy, where IgG was initially purified and used to generate anti-Fab specific antibodies. Immobilised anti-Fab specific antibodies were then used to capture other immunoglobulins from IgG depleted serum. While high quantities of IgM were successfully isolated from serum, IgA was not. Only trace quantities of IgA were detected in the serum by mass spectrometry. Immobilised ligands specific to IgA (Jacalin, Peptide M and staphylococcal superantigen-like protein) also failed to capture P. alecto IgA from serum. IgM was the second most abundant serum antibody after IgG. A survey of mucosal secretions found IgG was the dominant antibody class rather than IgA. Our study demonstrates healthy P. alecto bats have markedly less serum IgA than expected. Higher quantities of IgG in mucosal secretions may be compensation for this low abundance or lack of IgA. Knowledge and reagents developed within this study can be used in the future to examine class-specific antibody response within this important viral host.

Published

2013

30. Detection and measurement of carbohydrate deficient transferrin in serum using immuno-capture mass spectrometry: diagnostic applications for annual ryegrass toxicity and corynetoxin exposure.

Author

Penno MA, Colegate SM, Michalski WP, and Hoffmann P

Subjects

Animals, Biomarkers blood, Enzyme-Linked Immunosorbent Assay, Rats, Reproducibility of Results, Sensitivity and Specificity, Toxicity Tests, Chronic methods, Toxicity Tests, Chronic veterinary, Transferrin chemistry, Carbohydrates chemistry, Glycolipids chemistry, Lolium chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization methods, Transferrin metabolism

Abstract

The neurological livestock disease annual ryegrass toxicity (ARGT) is caused by the ingestion of the naturally occurring glycolipid toxins - the corynetoxins. Corynetoxins also threaten human health as potential contaminants of the food supply. Presently, there are no routine diagnostic tests for corynetoxins-exposure in humans or livestock. Chronic ingestion of corynetoxins has been modeled in rats exposed to dietary tunicamycins for 12 months and carbohydrate deficient transferrin (CDT) has been previously identified as a candidate disease biomarker. Here, the technique of immuno-capture mass spectrometry (icMS) was used to evaluate serum levels of CDT, discriminating between control and tunicamycins-exposed rats with 85% accuracy. The icMS approach is based on the combination of specific transferrin enrichment with functionalized magnetic beads and automated matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS). With no other clinically-relevant diagnostic tests available icMS could be readily adapted for high-throughput clinical assessment of corynetoxins-exposure in humans or livestock., (Copyright © 2012. Published by Elsevier India Pvt Ltd.)

Published

2012

31. Design and analysis of a multilayer localized surface plasmon resonance graphene biosensor.

Author

Islam MS, Kouzani AZ, Dai XJ, Michalski WP, and Gholamhosseini H

Subjects

Equipment Design, Equipment Failure Analysis, Nanostructures ultrastructure, Surface Properties, Biopolymers analysis, Biosensing Techniques instrumentation, Graphite chemistry, Immunoassay instrumentation, Nanostructures chemistry, Surface Plasmon Resonance instrumentation

Abstract

This paper describes a multilayer localized surface plasmon resonance (LSPR) graphene biosensor that includes a layer of graphene sheet on top of the gold layer, and the use of different coupled configuration of a laser beam. The study also investigates the enhancement of the sensitivity and detection accuracy of the biosensor through monitoring biomolecular interactions of biotin-streptavidin with the graphene layer on the gold thin film. Additionally, the role of thin films of gold, silver, copper and aluminum in the performance of the biosensor is separately investigated for monitoring the binding of streptavidin to the biotin groups. The performance of the LSPR graphene biosensor is theoretically and numerically assessed in terms of sensitivity, adsorption efficiency, and detection accuracy under varying conditions, including the thickness of biomolecule layer, number of graphene layers and operating wavelength. Enhanced sensitivity and improved adsorption efficiency are obtained for the LSPR graphene biosensor in comparison with its conventional counterpart; however, detection accuracy under the same resonance condition is reduced by 5.2% with a single graphene sheet. This reduction in detection accuracy (signal to noise ratio) can be compensated for by introducing an additional layer of silica doped B2O3 (sdB2O3) placed under the graphene layer. The role of prism configuration, prism angle and the interface medium (air and water) is also analyzed and it is found that the LSPR graphene biosensor has better sensitivity with triangular prism, higher prism angle, lower operating wavelength and larger number of graphene layers. The approach involves a plot of a reflectivity curve as a function of the incidence angle. The outcomes of this investigation highlight the ideal functioning condition corresponding to the best design parameters.

Published

2012

32. Correlation between spatial (3D) structure of pea and bean thylakoid membranes and arrangement of chlorophyll-protein complexes.

Author

Rumak I, Mazur R, Gieczewska K, Kozioł-Lipińska J, Kierdaszuk B, Michalski WP, Shiell BJ, Venema JH, Vredenberg WJ, Mostowska A, and Garstka M

Subjects

Chlorophyll metabolism, Chlorophyll A, Kinetics, Light-Harvesting Protein Complexes metabolism, Membrane Proteins metabolism, Mesophyll Cells cytology, Mesophyll Cells ultrastructure, Microscopy, Confocal, Photosystem I Protein Complex metabolism, Photosystem II Protein Complex metabolism, Plant Leaves metabolism, Plant Proteins metabolism, Protein Denaturation, Spectrometry, Fluorescence, Temperature, Thylakoids metabolism, Chlorophyll Binding Proteins metabolism, Imaging, Three-Dimensional methods, Pisum sativum metabolism, Pisum sativum ultrastructure, Phaseolus metabolism, Phaseolus ultrastructure, Thylakoids ultrastructure

Abstract

Background: The thylakoid system in plant chloroplasts is organized into two distinct domains: grana arranged in stacks of appressed membranes and non-appressed membranes consisting of stroma thylakoids and margins of granal stacks. It is argued that the reason for the development of appressed membranes in plants is that their photosynthetic apparatus need to cope with and survive ever-changing environmental conditions. It is not known however, why different plant species have different arrangements of grana within their chloroplasts. It is important to elucidate whether a different arrangement and distribution of appressed and non-appressed thylakoids in chloroplasts are linked with different qualitative and/or quantitative organization of chlorophyll-protein (CP) complexes in the thylakoid membranes and whether this arrangement influences the photosynthetic efficiency., Results: Our results from TEM and in situ CLSM strongly indicate the existence of different arrangements of pea and bean thylakoid membranes. In pea, larger appressed thylakoids are regularly arranged within chloroplasts as uniformly distributed red fluorescent bodies, while irregular appressed thylakoid membranes within bean chloroplasts correspond to smaller and less distinguished fluorescent areas in CLSM images. 3D models of pea chloroplasts show a distinct spatial separation of stacked thylakoids from stromal spaces whereas spatial division of stroma and thylakoid areas in bean chloroplasts are more complex. Structural differences influenced the PSII photochemistry, however without significant changes in photosynthetic efficiency. Qualitative and quantitative analysis of chlorophyll-protein complexes as well as spectroscopic investigations indicated a similar proportion between PSI and PSII core complexes in pea and bean thylakoids, but higher abundance of LHCII antenna in pea ones. Furthermore, distinct differences in size and arrangements of LHCII-PSII and LHCI-PSI supercomplexes between species are suggested., Conclusions: Based on proteomic and spectroscopic investigations we postulate that the differences in the chloroplast structure between the analyzed species are a consequence of quantitative proportions between the individual CP complexes and its arrangement inside membranes. Such a structure of membranes induced the formation of large stacked domains in pea, or smaller heterogeneous regions in bean thylakoids. Presented 3D models of chloroplasts showed that stacked areas are noticeably irregular with variable thickness, merging with each other and not always parallel to each other.

Published

2012

33. Site occupancy and glycan compositional analysis of two soluble recombinant forms of the attachment glycoprotein of Hendra virus.

Author

Colgrave ML, Snelling HJ, Shiell BJ, Feng YR, Chan YP, Bossart KN, Xu K, Nikolov DB, Broder CC, and Michalski WP

Subjects

Amino Acid Motifs, Amino Acid Sequence, Carbohydrate Conformation, Carbohydrate Sequence, Crystallography, X-Ray, Electrophoretic Mobility Shift Assay, Glycosylation, HEK293 Cells, HeLa Cells, Humans, Lectins chemistry, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Protein Binding, Protein Structure, Quaternary, Receptor, EphB2 chemistry, Recombinant Proteins chemistry, Sequence Analysis, Protein, Hendra Virus, Polysaccharides chemistry, Viral Envelope Proteins chemistry

Abstract

Hendra virus (HeV) continues to cause morbidity and mortality in both humans and horses with a number of sporadic outbreaks. HeV has two structural membrane glycoproteins that mediate the infection of host cells: the attachment (G) and the fusion (F) glycoproteins that are essential for receptor binding and virion-host cell membrane fusion, respectively. N-linked glycosylation of viral envelope proteins are critical post-translation modifications that have been implicated in roles of structural integrity, virus replication and evasion of the host immune response. Deciphering the glycan composition and structure on these glycoproteins may assist in the development of glycan-targeted therapeutic intervention strategies. We examined the site occupancy and glycan composition of recombinant soluble G (sG) glycoproteins expressed in two different mammalian cell systems, transient human embryonic kidney 293 (HEK293) cells and vaccinia virus (VV)-HeLa cells, using a suite of biochemical and biophysical tools: electrophoresis, lectin binding and tandem mass spectrometry. The N-linked glycans of both VV and HEK293-derived sG glycoproteins carried predominantly mono- and disialylated complex-type N-glycans and a smaller population of high mannose-type glycans. All seven consensus sequences for N-linked glycosylation were definitively found to be occupied in the VV-derived protein, whereas only four sites were found and characterized in the HEK293-derived protein. We also report, for the first time, the existence of O-linked glycosylation sites in both proteins. The striking characteristic of both proteins was glycan heterogeneity in both N- and O-linked sites. The structural features of G protein glycosylation were also determined by X-ray crystallography and interactions with the ephrin-B2 receptor are discussed.

Published

2012

34. Production and proteomic characterisation of purified protein derivative from Mycobacterium avium subsp. paratuberculosis.

Author

Wynne JW, Shiell BJ, Colgrave ML, Vaughan JA, Beddome G, and Michalski WP

Abstract

Background: Effective diagnosis of Johne's disease (JD), particularly at the stage of early subclinical infection, remains one of the greatest challenges for the control of JD worldwide. The IFN-γ test of cell mediated immunity is currently one of the most suitable diagnostics for subclinical infections, however a major limitation of this test is the lack of a standardised purified protein derivative (PPD) antigen (also referred to as Johnin PPD or PPDj). While attempting to replace PPDj with more specific individual antigens is an attractive proposition, bacterial culture derived PPDj remains the most effective antigen preparation for the diagnosis of subclinical JD. It may be possible to increase the reproducibility and specificity of PPDj preparations by further characterising and standardising the PPDj production., Results: Using a standardised protocol, five in-house preparations of PPDj were prepared from cultures of Mycobacterium avium subsp. paratuberculosis (MAP). Compared to PPDs obtained from other institutes/laboratories, these preparations appeared to perform similarly well in the IFN-γ test. Although the broad proteomic composition of all PPDj preparations was remarkably similar, the absolute abundance of individual proteins varied markedly between preparations. All PPDj preparations contained common immunogenic proteins which were also observed in PPD preparations from Mycobacterium avium subsp. avium (PPDa) and Mycobacterium bovis (PPDb). Temporal difference in protein secretion of in vitro cultured MAP was observed between 20 and 34 weeks suggesting that the age of MAP culture used for PPDj preparations may markedly influence PPDj composition., Conclusions: This study describes a protocol for the production of PPDj and its subsequent proteomic characterisation. The broad proteomic composition of different preparations of PPDj was, for the most part, highly similar. Compositional differences between PPDj preparations were found to be a direct reflection of genetic differences between the MAP strain types used to produce these preparations and the age of MAP cultures they were derived from. A number of conserved immunogenic proteins, such as members of the cutinase-like protein family, were found to be more abundant in PPDj compared to PPDa and should be considered as possible diagnostic antigens for the future.

Published

2012

35. Peptides specific for Mycobacterium avium subspecies paratuberculosis infection: diagnostic potential.

Author

Casey JL, Sanalla AM, Tamvakis D, Thalmann C, Carroll EL, Parisi K, Coley AM, Stewart DJ, Vaughan JA, Michalski WP, Luke R, and Foley M

Subjects

Amino Acid Sequence, Animals, Antibodies, Bacterial blood, Antigens, Bacterial metabolism, Bacterial Proteins metabolism, Biomarkers blood, Epitopes, Goats, Molecular Sequence Data, Mycobacterium avium subsp. paratuberculosis isolation & purification, Paratuberculosis microbiology, Peptide Library, Peptides metabolism, Predictive Value of Tests, Rabbits, Serologic Tests methods, Bacterial Typing Techniques methods, Mycobacterium avium subsp. paratuberculosis metabolism, Paratuberculosis diagnosis

Abstract

Mycobacterium avium subspecies paratuberculosis (Map) is the causative agent of Johne's disease (JD). Current serological diagnostic tests for JD are limited by their sensitivity when used in sub-clinical stages of the disease. Our objective was to identify peptides that mimic diagnostically important Map epitopes that might be incorporated into a new-generation JD diagnostic. Four peptides were isolated from a phage-displayed random peptide library by screening on antibodies derived from Map-infected goats. The peptides were recognised by antibodies from Map-infected goats but not by antibodies from uninfected goats. The peptides elicited immune responses in rabbits, which reacted strongly with bona fide Map antigens proving the peptides were true epitope mimics. To assess the diagnostic value a panel of goat sera was screened for reactivity's with peptides. The peptides were recognised by antibodies from a proportion of goats infected with Map compared with control animals with a diagnostic specificity of 100% and the sensitivity ranged from 50 to 75%. Combinations of any two peptides improved sensitivity 62.5-87.5% and 100% sensitivity was achieved with three of the four peptides in combination. These data suggest peptides representing diagnostically important Map epitopes could be incorporated into a sensitive diagnostic test.

Published

2011

36. Controlling cell growth on titanium by surface functionalization of heptylamine using a novel combined plasma polymerization mode.

Author

Zhao JH, Michalski WP, Williams C, Li L, Xu HS, Lamb PR, Jones S, Zhou YM, and Dai XJ

Subjects

Actins chemistry, Animals, Cell Line, Cell Proliferation, Cytoskeleton chemistry, Fibroblasts cytology, Mice, Microscopy, Fluorescence methods, Osseointegration, Osteoblasts cytology, Polymerization, Surface Properties, Amines chemistry, Biocompatible Materials chemistry, Titanium chemistry

Abstract

A novel bio-interface, produced by a combined plasma polymerization mode on a titanium (Ti) surface, was shown to enhance osteoblast growth and reduce fibroblast cell growth. This new method can securely attach a tailored interface to difficult materials such as Ti or ceramics. Here a more stable and higher density of NH₂ functional groups is able to withstand sterilization in ethanol. The biocompatibility, in terms of cell attachment and actin cytoskeleton development, was markedly improved in vitro, compared with untreated Ti surfaces and samples treated by other plasma modes. It gave a boosted (approximately six times higher) cellular response of osteoblasts in their initial adhesion stage. These factors should increase the formation of new bone around implants (reducing healing time), promoting osseointegration and thereby increasing implantation success rates., (Copyright © 2011 Wiley Periodicals, Inc.)

Published

2011

37. Comparison of performance parameters for conventional and localized surface plasmon resonance graphene biosensors.

Author

Islam MS, Kouzani AZ, Dai XJ, Michalski WP, and Gholamhosseini H

Subjects

Equipment Design, Equipment Failure Analysis, Reproducibility of Results, Sensitivity and Specificity, Biopolymers analysis, Biosensing Techniques instrumentation, Graphite chemistry, Immunoassay instrumentation, Surface Plasmon Resonance instrumentation

Abstract

This paper investigates the enhancement of the sensitivity and adsorption efficiency of a localized surface plasmon resonance (LSPR) biosensor that includes a layer of graphene sheet on top of the gold layer. For this purpose, biomolecular interactions of biotin-streptavidin with the graphene layer on the gold thin film are monitored. The performance of the LSPR graphene biosensor is theoretically and numerically assessed in terms of sensitivity and adsorption efficiency under varying conditions, including the thickness of biomolecule layer, number of graphene layers and operating wavelength. Enhanced sensitivity and improved adsorption efficiency are obtained for the LSPR graphene biosensor in comparison with its conventional counterpart. It is found that the LSPR graphene biosensor has better sensitivity with lower operating wavelength and larger number of graphene layers.

Published

2011

38. Exploring the zoonotic potential of Mycobacterium avium subspecies paratuberculosis through comparative genomics.

Author

Wynne JW, Bull TJ, Seemann T, Bulach DM, Wagner J, Kirkwood CD, and Michalski WP

Subjects

Animals, Base Sequence, Cattle, Child, Crohn Disease microbiology, Gene Duplication genetics, High-Throughput Nucleotide Sequencing, Humans, Molecular Sequence Data, Mycobacterium avium subsp. paratuberculosis physiology, Paratuberculosis microbiology, Paratuberculosis transmission, Phylogeny, Polymorphism, Single Nucleotide genetics, Comparative Genomic Hybridization, Disease Transmission, Infectious, Genome, Bacterial genetics, Mycobacterium avium subsp. paratuberculosis genetics

Abstract

A comparative genomics approach was utilised to compare the genomes of Mycobacterium avium subspecies paratuberculosis (MAP) isolated from early onset paediatric Crohn's disease (CD) patients as well as Johne's diseased animals. Draft genome sequences were produced for MAP isolates derived from four CD patients, one ulcerative colitis (UC) patient, and two non-inflammatory bowel disease (IBD) control individuals using Illumina sequencing, complemented by comparative genome hybridisation (CGH). MAP isolates derived from two bovine and one ovine host were also subjected to whole genome sequencing and CGH. All seven human derived MAP isolates were highly genetically similar and clustered together with one bovine type isolate following phylogenetic analysis. Three other sequenced isolates (including the reference bovine derived isolate K10) were genetically distinct. The human isolates contained two large tandem duplications, the organisations of which were confirmed by PCR. Designated vGI-17 and vGI-18 these duplications spanned 63 and 109 open reading frames, respectively. PCR screening of over 30 additional MAP isolates (3 human derived, 27 animal derived and one environmental isolate) confirmed that vGI-17 and vGI-18 are common across many isolates. Quantitative real-time PCR of vGI-17 demonstrated that the proportion of cells containing the vGI-17 duplication varied between 0.01 to 15% amongst isolates with human isolates containing a higher proportion of vGI-17 compared to most animal isolates. These findings suggest these duplications are transient genomic rearrangements. We hypothesise that the over-representation of vGI-17 in human derived MAP strains may enhance their ability to infect or persist within a human host by increasing genome redundancy and conferring crude regulation of protein expression across biologically important regions.

Published

2011

39. RNA-binding domain in the nucleocapsid protein of gill-associated nidovirus of penaeid shrimp.

Author

Soowannayan C, Cowley JA, Michalski WP, and Walker PJ

Subjects

Amino Acid Sequence, Animals, Bacteriophage M13 genetics, Binding Sites genetics, Blotting, Western, Bunyaviridae genetics, DNA, Single-Stranded genetics, DNA, Single-Stranded metabolism, Electrophoretic Mobility Shift Assay, Gills virology, Molecular Sequence Data, Nucleocapsid Proteins genetics, Protein Binding, RNA genetics, RNA, Viral genetics, RNA, Viral metabolism, Roniviridae genetics, Nucleocapsid Proteins metabolism, Penaeidae virology, RNA metabolism, Roniviridae metabolism

Abstract

Gill-associated virus (GAV) infects Penaeus monodon shrimp and is the type species okavirus in the Roniviridae, the only invertebrate nidoviruses known currently. Electrophoretic mobility shift assays (EMSAs) using His(6)-tagged full-length and truncated proteins were employed to examine the nucleic acid binding properties of the GAV nucleocapsid (N) protein in vitro. The EMSAs showed full-length N protein to bind to all synthetic single-stranded (ss)RNAs tested independent of their sequence. The ssRNAs included (+) and (-) sense regions of the GAV genome as well as a (+) sense region of the M RNA segment of Mourilyan virus, a crustacean bunya-like virus. GAV N protein also bound to double-stranded (ds)RNAs prepared to GAV ORF1b gene regions and to bacteriophage M13 genomic ssDNA. EMSAs using the five N protein constructs with variable-length N-terminal and/or C-terminal truncations localized the RNA binding domain to a 50 amino acid (aa) N-terminal sequence spanning Met(11) to Arg(60). Similarly to other RNA binding proteins, the first 16 aa portion of this sequence was proline/arginine rich. To examine this domain in more detail, the 18 aa peptide (M(11)PVRRPLPPQPPRNARLI(29)) encompassing this sequence was synthesized and found to bind nucleic acids similarly to the full-length N protein in EMSAs. The data indicate a fundamental role for the GAV N protein proline/arginine-rich domain in nucleating genomic ssRNA to form nucleocapsids. Moreover, as the synthetic peptide formed higher-order complexes in the presence of RNA, the domain might also play some role in protein/protein interactions stabilizing the helical structure of GAV nucleocapsids.

Published

2011

40. Resequencing the Mycobacterium avium subsp. paratuberculosis K10 genome: improved annotation and revised genome sequence.

Author

Wynne JW, Seemann T, Bulach DM, Coutts SA, Talaat AM, and Michalski WP

Subjects

Molecular Sequence Data, Sequence Analysis, DNA methods, DNA, Bacterial chemistry, DNA, Bacterial genetics, Genome, Bacterial, Mycobacterium avium subsp. paratuberculosis genetics

Abstract

We report the resequencing and revised annotation of the Mycobacterium avium subsp. paratuberculosis K10 genome. A total of 90 single-nucleotide errors and a 51-bp indel in the original K10 genome were corrected, and the whole genome annotation was revised. Correction of these sequencing errors resulted in 28 frameshift alterations. The amended genome sequence is accessible via the supplemental section of study SRR060191 in the NCBI Sequence Read Archive and will serve as a valuable reference genome for future studies.

Published

2010

41. Glycosylation of gp116 and gp64 envelope proteins of yellow head virus of Penaeus monodon shrimp.

Author

Soowannayan C, Cowley JA, Pearson RD, Wallis TP, Gorman JJ, Michalski WP, and Walker PJ

Subjects

Amino Acid Sequence, Animals, Electrophoresis, Polyacrylamide Gel, Glycosylation, Mass Spectrometry, Molecular Sequence Data, Peptide-N4-(N-acetyl-beta-glucosaminyl) Asparagine Amidase metabolism, Roniviridae chemistry, Staining and Labeling methods, Viral Envelope Proteins isolation & purification, Penaeidae virology, Protein Processing, Post-Translational, Roniviridae physiology, Viral Envelope Proteins metabolism

Abstract

Yellow head virus (YHV) is a highly virulent pathogen of Penaeus monodon shrimp that is classified in the genus Okavirus, family Roniviridae, in the order Nidovirales. Separation of virion proteins treated with peptide-N-glycosidase-F (PNGase-F) in SDS-polyacrylamide gels and the use of glycoprotein-specific staining methods indicated that the gp116 and gp64 envelope glycoproteins possess N-linked rather than O-linked glycans. Competitive binding inhibition of lectins with various oligosaccharide specificities indicated that glycans linked to gp64 are mannose-rich, whilst glycans linked to gp116 possess terminal N-acetylgalactosamine and N-acetylglucosamine in addition to terminal mannose-type sugars. Mass spectrometry analyses of peptides generated from YHV proteins before and after deglycosylation with PNGase-F, using combinations of the endoproteinases trypsin, Asp-N and Lys-C, confirmed occupancy of six of the seven potential N-linked glycosylation sites in gp116 and three of the four potential sites in gp64.

Published

2010

42. 3-D modeling of a carbon nanotube cantilever biosensor.

Author

Islam SM, Kouzani AZ, Dai XJ, and Michalski WP

Subjects

Models, Theoretical, Biosensing Techniques instrumentation, Biosensing Techniques methods, Nanotubes, Carbon, Static Electricity

Abstract

In this paper, 3-D finite element modeling and simulations are carried out to investigate the bending deformation of a single-walled carbon nanotube cantilever biosensor due to mass attached, and addition of a nano-scale particles to the beam tip resulting from the bioparticle detection. In addition, an algorithm for an electrostatic-mechanical coupled system is developed. The computed results are in excellent agreement with the well known electrostatic equations that govern the deformation.

Published

2010

43. Off Label Antiviral Therapeutics for Henipaviruses: New Light Through Old Windows.

Author

Aljofan M, Lo MK, Rota PA, Michalski WP, and Mungall BA

Abstract

Hendra and Nipah viruses are recently emerged zoonotic paramyxoviruses for which there is no vaccine or protective therapy available. While a number of experimental therapeutics and vaccines have recently been reported, all of these will require lengthy approval processes, limiting their usefulness in the short term. To address the urgent need for henipavirus therapeutics, a number of currently licensed pharmaceuticals have been evaluated for off label efficacy against henipavirus replication in vitro. Initially it was observed that compounds which released intracellular calcium stores induced a potent inhibition of henipaviruses replication, prompting the evaluation of known drugs with a similar effect on calcium mobilisation. Of the eight compounds randomly selected based on existing literature, seven inhibited virus replication in the micromolar range while the remaining compound also inhibited virus replication but only at millimolar concentrations. Pretreatment experiments with various calcium chelators, channel antagonists or endoplasmic reticulum release inhibitors supported a calcium mediated mechanism of action for five of these compounds. The mechanism of antiviral action for the remaining three compounds is currently unknown. Additionally, a number of other modulators of calcium flux, including calcium channel and calmodulin antagonists also exhibited potent antiviral activity in vitro providing a broad range of potential therapeutic options for the treatment of henipavirus infections. Importantly, as many of these compounds are currently licensed drugs, regulatory approval should be a much more streamlined process, with the caveat that appropriate in vivo efficacy can be demonstrated in animal models.

Published

2010

44. Novel monoclonal antibodies against Menangle virus nucleocapsid protein.

Author

Zvirbliene A, Kucinskaite-Kodze I, Juozapaitis M, Lasickiene R, Gritenaite D, Russell G, Bingham J, Michalski WP, and Sasnauskas K

Subjects

Amino Acid Sequence, Animals, Antibodies, Monoclonal analysis, Epitope Mapping, Immunoassay methods, Immunoglobulin G analysis, Mice, Mice, Inbred BALB C, Molecular Sequence Data, Nucleocapsid Proteins chemistry, Nucleocapsid Proteins genetics, Paramyxoviridae Infections diagnosis, Paramyxoviridae Infections immunology, Paramyxoviridae Infections virology, Paramyxovirinae chemistry, Paramyxovirinae isolation & purification, Sequence Alignment, Swine, Swine Diseases diagnosis, Swine Diseases immunology, Antibodies, Monoclonal immunology, Immunoglobulin G immunology, Nucleocapsid Proteins immunology, Paramyxoviridae Infections veterinary, Paramyxovirinae immunology, Swine Diseases virology

Abstract

Menangle virus (MenV) is a member of the family Paramyxoviridae isolated in Australia that causes a reproductive disease of pigs. There is a need for specific immunoassays for virus detection to facilitate the diagnosis of MenV infection. Three novel monoclonal antibodies (MAbs) of the IgG1 subtype were generated by immunizing mice with recombinant yeast-expressed MenV nucleocapsid (N) protein self-assembled to nucleocapsid-like structures. One MAb was cross-reactive with recombinant N protein of Tioman virus. The epitopes of MAbs were mapped using a series of truncated MenV N proteins lacking the 29-119 carboxy-terminal amino acid (aa) residues. The epitopes of two MAbs were mapped to aa 430-460 of the MenV N protein, whilst the epitope of one MAb was mapped to residues 460-490. All three MAbs specifically recognized MenV, as indicated by immunohistochemical staining of brain tissue isolated from a field case (a stillborn piglet) of MenV infection. The MAbs against MenV N protein may be a useful tool for immunohistological diagnosis of MenV infection.

Published

2010

45. Establishment, immortalisation and characterisation of pteropid bat cell lines.

Author

Crameri G, Todd S, Grimley S, McEachern JA, Marsh GA, Smith C, Tachedjian M, De Jong C, Virtue ER, Yu M, Bulach D, Liu JP, Michalski WP, Middleton D, Field HE, and Wang LF

Subjects

Animals, Cell Shape drug effects, Cloning, Molecular, Hendra Virus drug effects, Hendra Virus physiology, Henipavirus Infections virology, Humans, Immunity, Innate drug effects, Immunity, Innate immunology, Interferons genetics, Nipah Virus drug effects, Nipah Virus physiology, Poly I-C pharmacology, Simian virus 40 genetics, Cell Culture Techniques methods, Cell Line, Transformed cytology, Chiroptera

Abstract

Background: Bats are the suspected natural reservoir hosts for a number of new and emerging zoonotic viruses including Nipah virus, Hendra virus, severe acute respiratory syndrome coronavirus and Ebola virus. Since the discovery of SARS-like coronaviruses in Chinese horseshoe bats, attempts to isolate a SL-CoV from bats have failed and attempts to isolate other bat-borne viruses in various mammalian cell lines have been similarly unsuccessful. New stable bat cell lines are needed to help with these investigations and as tools to assist in the study of bat immunology and virus-host interactions., Methodology/findings: Black flying foxes (Pteropus alecto) were captured from the wild and transported live to the laboratory for primary cell culture preparation using a variety of different methods and culture media. Primary cells were successfully cultured from 20 different organs. Cell immortalisation can occur spontaneously, however we used a retroviral system to immortalise cells via the transfer and stable production of the Simian virus 40 Large T antigen and the human telomerase reverse transcriptase protein. Initial infection experiments with both cloned and uncloned cell lines using Hendra and Nipah viruses demonstrated varying degrees of infection efficiency between the different cell lines, although it was possible to infect cells in all tissue types., Conclusions/significance: The approaches developed and optimised in this study should be applicable to bats of other species. We are in the process of generating further cell lines from a number of different bat species using the methodology established in this study.

Published

2009

46. Mycobacterium avium subspecies paratuberculosis in children with early-onset Crohn's disease.

Author

Kirkwood CD, Wagner J, Boniface K, Vaughan J, Michalski WP, Catto-Smith AG, Cameron DJ, and Bishop RF

Subjects

Adolescent, Age of Onset, Base Sequence, Biopsy, Child, Child, Preschool, DNA, Bacterial genetics, DNA, Bacterial metabolism, Female, Humans, Leukocytes, Mononuclear microbiology, Male, Microbiological Techniques, Molecular Sequence Data, Mycobacterium avium subsp. paratuberculosis genetics, Paratuberculosis blood, Paratuberculosis pathology, Polymerase Chain Reaction, Crohn Disease complications, Crohn Disease microbiology, Intestinal Mucosa microbiology, Intestinal Mucosa pathology, Mycobacterium avium subsp. paratuberculosis isolation & purification, Paratuberculosis complications

Abstract

Background: Mycobacterium avium subspecies paratuberculosis (MAP) is the most enduring infectious candidate that may be associated with inflammatory bowel disease (IBD). It is possible that the inconsistencies in the prevalence studies of MAP in adults reflect clinical differences in adult patients studied, including duration of disease and treatment regimens, and also in lack of specificity of some of the assays used. The aim was to determine the presence of MAP in children with symptoms of Crohn's disease (CD) and ulcerative colitis (UC), using gut biopsy tissue and peripheral blood mononuclear cells (PBMC) collected at initial endoscopic examination prior to clinical treatment., Methods: Mucosal biopsies and/or PBMC specimens were collected from a total of 142 children, comprising 62 with CD, 26 with UC, and 54 with non-IBD. MAP-specific IS900 polymerase chain reaction (PCR) analysis was performed on all biopsies and PBMC specimens. Conventional MAP culture technique was performed on a subset of 10 CD, 2 UC, and 4 non-IBD patients to isolate MAP., Results: MAP was identified by IS900 PCR significantly more often in mucosal biopsies from CD 39% (22/56) than from non-IBD 15% (6/39) patients (P < 0.05), and in PBMC from CD 16% (8/50) than from non-IBD 0% (0/31) patients (P < 0.05). Viable MAP were cultured from mucosal biopsies from 4/10 CD, 0/2 UC, and 0/4 non-IBD patients, but were not cultured from PBMC specimens., Conclusions: This unique study on the occurrence of MAP in gut tissue and blood from pediatric IBD patients suggests the possible involvement of MAP in the early stages of development of CD in children.

Published

2009

47. Generation of Tioman virus nucleocapsid-like particles in yeast Saccharomyces cerevisiae.

Author

Petraityte R, Tamosiunas PL, Juozapaitis M, Zvirbliene A, Sasnauskas K, Shiell B, Russell G, Bingham J, and Michalski WP

Subjects

Amino Acid Sequence, Animals, Antibodies, Viral immunology, Antigens, Viral immunology, Chiroptera, Immunohistochemistry, Mice, Microscopy, Electron, Transmission, Molecular Sequence Data, Nucleocapsid Proteins genetics, Nucleocapsid Proteins immunology, Nucleocapsid Proteins ultrastructure, Paramyxoviridae Infections immunology, Paramyxoviridae Infections virology, Pneumovirinae immunology, Pneumovirinae isolation & purification, Rabbits, Recombinant Proteins genetics, Recombinant Proteins immunology, Recombinant Proteins ultrastructure, Swine, Nucleocapsid Proteins biosynthesis, Pneumovirinae genetics, Recombinant Proteins biosynthesis, Saccharomyces cerevisiae metabolism

Abstract

Tioman virus (TioV) was isolated from a number of pooled urine samples of Tioman Island flying foxes (Pteropus hypomelanus) during the search for the reservoir host of Nipah virus. Studies have established TioV as a new virus in the family Paramyxoviridae. This novel paramyxovirus is antigenically related to Menangle virus that was isolated in Australia in 1997 during disease outbreak in pigs. TioV causes mild disease in pigs and has a predilection for lymphoid tissues. Recent serosurvey showed that 1.8% of Tioman Islanders had neutralizing antibodies against TioV, indicating probable past infection. For the development of convenient serological tests for this virus, recombinant TioV nucleocapsid (N) protein was expressed in the yeast Saccharomyces cerevisiae. High yields of recombinant TioV N protein were obtained. Electron microscopy demonstrated that purified recombinant N protein self-assembled into nucleocapsid-like particles which were identical in density and morphology to authentic nucleocapsids from paramyxovirus-infected cells. Different size nucleocapsid-like particles were stable and readily purified by CsCl gradient ultracentrifugation. Polyclonal sera raised in rabbits after immunization with recombinant TioV N protein reacted reliably with TioV infected tissues in immunohistochemistry tests. It confirmed that the antigenic properties of yeast derived TioV N protein are identical to authentic viral protein.

Published

2009

48. Identifying candidate serum biomarkers of exposure to tunicamycins in rats using two-dimensional electrophoresis.

Author

Penno MA, Bacic A, Colegate SM, Hoffmann P, and Michalski WP

Subjects

Amino Acid Sequence, Analysis of Variance, Animals, Female, Glycolipids administration & dosage, Glycolipids toxicity, Glycosylation, Male, Molecular Sequence Data, Rats, Tandem Mass Spectrometry, Transferrin metabolism, Tunicamycin administration & dosage, Tunicamycin metabolism, Biomarkers blood, Blood Proteins metabolism, Electrophoresis, Gel, Two-Dimensional methods, Proteome metabolism, Toxicity Tests, Chronic methods, Tunicamycin toxicity

Abstract

A model for chronic corynetoxins poisoning has been established in rats exposed to the toxicologically bioequivalent inhibitor of N-linked glycosylation the tunicamycins. Consumption of corynetoxins in contaminated pasture can result in the often fatal neurological disease of grazing livestock annual ryegrass toxicity (ARGT). Corynetoxins may also threaten human health as potential contaminants of the food supply via grain or products derived from subclinically exposed animals. The serum proteomes of four dose groups plus a control group following 6, 9, and 12 months dietary tunicamycins exposure were compared by one-dimensional electrophoresis. Numerous differences were observed between the control and the highest dose group (40.5 mug tunicamycins/kg of body weight/day), designated as High). Accordingly, these samples were further examined using two-dimensional electrophoresis. Thirty-three protein spots were found to be differentially displayed between the Control and High dose sera based on univariate statistics (p < 0.05 for log(10) transformed normalized volumes) and significant fold-changes in spot volume (+/-2.3-fold as determined by posthoc power analysis). Identities for 28 spots were obtained by MALDI-TOF MS corresponding to 13 different proteins. An increasing population of carbohydrate deficient transferrin was identified in the High dose sera using a combination of antibody and lectin detection and confirmed by ESI-IT MS/MS. The functionalities of other identified proteins were consistent with the oxidative stress and acute phase responses. The biomarkers identified in this study may not only play a useful role in diagnosing toxin exposure but could be helpful in identifying new treatment strategies for ARGT and equivalent human diseases.

Published

2009

49. The recovery of Mycobacterium avium subspecies paratuberculosis from the intestine of infected ruminants for proteomic evaluation.

Author

Egan S, Lanigan M, Shiell B, Beddome G, Stewart D, Vaughan J, and Michalski WP

Subjects

Animals, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins metabolism, Cattle, Electrophoresis, Gel, Two-Dimensional, Molecular Sequence Data, Mycobacterium avium subsp. paratuberculosis chemistry, Mycobacterium avium subsp. paratuberculosis genetics, Mycobacterium avium subsp. paratuberculosis metabolism, Cattle Diseases microbiology, Intestines microbiology, Mycobacterium avium subsp. paratuberculosis isolation & purification, Paratuberculosis microbiology, Proteomics

Abstract

Johne's disease is a slowly developing intestinal disease, primarily of ruminants, caused by Mycobacterium avium subspecies paratuberculosis. The disease contributes to significant economic losses worldwide in agricultural industry. Analysis of bacterial proteomes isolated directly from infected animals can provide important information about the repertoire of proteins present during infection and disease progression. In this study, M. avium subspecies paratuberculosis has been extracted from Johne's disease-infected cattle and goat intestinal tissue sections in a manner compatible with direct 2-DE proteomic analysis for comparison with in vitro-cultured bacteria. M. avium subspecies paratuberculosis was harvested from the submucosa and mucosa of intestinal sections and enriched from macerated tissue by hypotonic lysis, sonication and centrifugation through a viscosity gradient. Subsequent comparison of the proteomes of the in vivo- and in vitro-derived bacteria identified a number of proteins that were differentially expressed. Among them, a number of hypothetical proteins of unknown function and a hypothetical fatty acyl dehydrogenase (FadE3&#95;2) and 3-hydroxyacyl-CoA dehydrogenase, possibly important for in vivo metabolism, utilising the pathway for the beta-oxidation of fatty acids.

Published

2008

50. Bohle iridovirus as a vector for heterologous gene expression.

Author

Pallister J, Goldie S, Coupar B, Shiell B, Michalski WP, Siddon N, and Hyatt A

Subjects

Animals, Cell Line, DNA, Recombinant genetics, Globins biosynthesis, Larva virology, Recombinant Proteins biosynthesis, Bufo marinus genetics, Gene Expression, Genetic Vectors, Globins genetics, Ranavirus genetics

Abstract

The large double-stranded DNA (ds DNA) viruses were among the first to be used to construct recombinant viruses, but to date this has not been achieved with any members of the ds DNA virus family, Iridoviridae. We identified a non-essential gene, the viral homologue of eukaryotic initiation factor 2alpha (eIF-2alpha), in Bohle iridovirus (BIV, genus Ranavirus). A recombinant BIV was constructed with the neomycin resistance gene and the Bufo marinus (cane toad) adult globin gene inserted into the BIV eIF-2alpha region. Adult globin expressed by the virus was detected on western blot, demonstrating that foreign genes can be expressed by the recombinant BIV in vitro and suggesting the possibility of using a recombinant BIV in the biological control of cane toads.

Published

2007