Your search keyword '"Brian A. Crowe"' showing total 45 results

1. Modulation of the liver immune microenvironment by the adeno-associated virus serotype 8 gene therapy vector

Author

Agostina Carestia, Seok-Joo Kim, Franziska Horling, Hanspeter Rottensteiner, Christian Lubich, Birgit M. Reipert, Brian A. Crowe, and Craig N. Jenne

Subjects

Adeno-associated virus-8, gene therapy, liver, immune response, intravital imaging, inflammation, Genetics, QH426-470, Cytology, QH573-671

Abstract

Adeno-associated viruses (AAVs) are emerging as one of the vehicles of choice for gene therapy. However, the potential immunogenicity of these vectors is a major limitation of their use, leading to the necessity of a better understanding of how viral vectors engage the innate immune system. In this study, we demonstrate the immune response mediated by an AAV vector in a mouse model. Mice were infected intravenously with 4 × 1012 copies (cp)/kg of AAV8, and the ensuing immune response was analyzed using intravital microscopy during a period of weeks. Administration of AAV8 resulted in the infection of hepatocytes, and this infection led to a moderate, but significant, activation of the immune system in the liver. This host immune response involved platelet aggregation, neutrophil extracellular trap (NET) formation, and the recruitment of monocytes, B cells, and T cells. The resident liver macrophage population, Kupffer cells, was necessary to initiate this immune response, as its depletion abrogated platelet aggregation and NET formation and delayed the recruitment of immune cells. Moreover, the death of liver cells produced by this AAV was moderate and failed to result in a robust, sustained inflammatory response. Altogether, these data suggest that AAV8 is a suitable vector for gene therapy approaches.

Published

2021

2. Comprehensive approach for identification of functional FCGR2C alleles resulting in protein expression as a determinant for predicting predisposition to autoimmunity

Author

Dorit Lehmann, Sabine Unterthurner, Verena Berg, Karin Hock, Padmapriya Ponnuswamy, Mantas Malisauskas, Brian A. Crowe, Bekir Erguener, Christoph Bock, Greg Hather, Birgit M. Reipert, and Ivan Bilic

Subjects

copy number variation, FCGR2C expression, low affinity immunoglobulin receptors, SNP, systemic lupus erythematosus, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract The balance of activating and inhibitory signals from the low affinity Fc gamma receptors modulates immune responses triggered by IgG antibody‐immune complexes. In homeostasis, this leads to antigen clearance, while in autoimmune diseases to unwanted immune response. Besides the activating receptors FcɣRIIa, FcɣRIIIa, and the inhibitory FcɣRIIb receptor, a third activating receptor, FcɣRIIc, was shown to be expressed on several immune cell types, however, only in the presence of a functional FCGR2C‐ORF allele. FcɣRIIc expression is associated with autoimmune diseases such as idiopathic thrombocytopenic purpura, systemic lupus erythematosus or systemic sclerosis. Thus, the determination of the functional FCGR2C gene resulting in protein expression on immune cells becomes highly relevant, particularly in the context of unwanted immune responses through inadvertent FcɣRIIc activation by molecules targeting stimulation of the inhibitory receptor FcɣRIIb, currently pursued by several pharmaceutical companies. The high degree of homology within the FCGR2/3 gene cluster complicates development of an accurate method for identification of FcɣRIIc expression. Here we describe a comprehensive approach to characterize genetic status of the FCGR2C gene locus consisting of cDNA sequencing, SNaPshot genotyping and low‐coverage next‐generation sequencing. This might enable Mendelian randomization hypothesis testing across autoimmune diseases to personalize therapies and enhance treatment outcomes.

Published

2021

3. The soluble cytoplasmic tail of CD45 regulates T‐cell activation via TLR4 signaling

Author

Alexander Puck, Katharina Radakovics, Birgit M. Reipert, Madhura Modak, Peter Steinberger, Brian A. Crowe, Sarojinidevi Künig, Johannes Stöckl, Claire Battin, Lara May, and Pia Fritz

Subjects

Reporter gene, T-Lymphocytes, T cell, Immunology, NFAT, Biology, Lymphocyte Activation, Jurkat cells, Cell biology, Toll-Like Receptor 4, Jurkat Cells, TLR2, medicine.anatomical_structure, Downregulation and upregulation, Cell culture, medicine, Humans, Leukocyte Common Antigens, Immunology and Allergy, Transcription factor, Cell Proliferation, Signal Transduction

Abstract

The soluble cytoplasmic tail of CD45 (ct-CD45) is a cleavage fragment of CD45, that is generated during the activation of human phagocytes. Upon release to the extracellular space, ct-CD45 binds to human T cells and inhibits their activation in vitro. Here, we studied the potential role of TLR4 as a receptor for ct-CD45. Treatment of Jurkat TLR4/CD14 reporter cells with ct-CD45 induced the upregulation of the reporter gene NFκB-eGFP and could be blocked by inhibitors of TLR4 signaling. Conversely, ct-CD45 did not promote the NFκB-controlled eGFP induction in reporter cells expressing TLR1, TLR2, and TLR6 transgenes and did not lead to the activation of the transcription factors NFκB, AP-1, and NFAT in a Jurkat reporter cell line expressing endogenous TLR5. Moreover, ct-CD45 binds to recombinant TLR4 in an in vitro assay and this association was reduced in the presence of oxidized 1-palmitoyl-2-arachidonyl-sn-glycero-3-phosphorylcholine. Blockade of TLR4 with mAb HTA125 partially reversed the ct-CD45-mediated inhibition of T-cell proliferation. Interestingly, targeting of TLR4 with mAb W7C11 also suppressed T-cell proliferation. In summary, the results of this study demonstrate that ct-CD45 acts via a noncanonical TLR4 activation pathway on T cells, which modulates TCR signaling.

Published

2021

4. Modulation of the liver immune microenvironment by the adeno-associated virus serotype 8 gene therapy vector

Author

Birgit M. Reipert, Franziska Horling, Christian Lubich, Seok-Joo Kim, Agostina Carestia, Craig N. Jenne, Brian A. Crowe, and Hanspeter Rottensteiner

Subjects

0301 basic medicine, lcsh:QH426-470, Genetic enhancement, Population, Inflammation, Biology, medicine.disease_cause, liver, immune response, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Immune system, Genetics, medicine, Adeno-associated virus-8, lcsh:QH573-671, education, Molecular Biology, Adeno-associated virus, education.field_of_study, Innate immune system, lcsh:Cytology, Immunogenicity, gene therapy, lcsh:Genetics, 030104 developmental biology, inflammation, 030220 oncology & carcinogenesis, Immunology, Molecular Medicine, Original Article, intravital imaging, medicine.symptom

Abstract

Adeno-associated viruses (AAVs) are emerging as one of the vehicles of choice for gene therapy. However, the potential immunogenicity of these vectors is a major limitation of their use, leading to the necessity of a better understanding of how viral vectors engage the innate immune system. In this study, we demonstrate the immune response mediated by an AAV vector in a mouse model. Mice were infected intravenously with 4 × 1012 copies (cp)/kg of AAV8, and the ensuing immune response was analyzed using intravital microscopy during a period of weeks. Administration of AAV8 resulted in the infection of hepatocytes, and this infection led to a moderate, but significant, activation of the immune system in the liver. This host immune response involved platelet aggregation, neutrophil extracellular trap (NET) formation, and the recruitment of monocytes, B cells, and T cells. The resident liver macrophage population, Kupffer cells, was necessary to initiate this immune response, as its depletion abrogated platelet aggregation and NET formation and delayed the recruitment of immune cells. Moreover, the death of liver cells produced by this AAV was moderate and failed to result in a robust, sustained inflammatory response. Altogether, these data suggest that AAV8 is a suitable vector for gene therapy approaches., Graphical Abstract, Using intravital microscopy, the immune response to AAV8 infection was assessed. Viral infection of hepatocytes led to a transient increase of platelet aggregation and NET formation. Interestingly, acute infection resulted in a reprograming of Kupffer cells to a pro-inflammatory state (CD80+CD206−) that returned to a baseline phenotype 3–4 weeks post-infection.

Published

2020

5. Author response for 'The soluble cytoplasmic tail of CD45 regulates T cell activation via TLR4 signaling'

Author

Claire Battin, Sarojinidevi Künig, Katharina Radakovics, Brian A. Crowe, Alexander Puck, Lara May, Peter Steinberger, Johannes Stöckl, Pia Fritz, Birgit M. Reipert, and Madhura Modak

Subjects

medicine.anatomical_structure, Cytoplasm, T cell, medicine, Tlr4 signaling, Biology, Cell biology

Published

2021

6. MVA vectors expressing conserved influenza proteins protect mice against lethal challenge with H5N1, H9N2 and H7N1 viruses.

Author

Annett Hessel, Helga Savidis-Dacho, Sogue Coulibaly, Daniel Portsmouth, Thomas R Kreil, Brian A Crowe, Michael G Schwendinger, Andreas Pilz, P Noel Barrett, Falko G Falkner, and Birgit Schäfer

Subjects

Medicine, Science

Abstract

BACKGROUND: The availability of a universal influenza vaccine able to induce broad cross-reactive immune responses against diverse influenza viruses would provide an alternative to currently available strain-specific vaccines. We evaluated the ability of vectors based on modified vaccinia virus Ankara (MVA) expressing conserved influenza proteins to protect mice against lethal challenge with multiple influenza subtypes. METHODS: Mice were immunized with MVA vectors expressing H5N1-derived nucleoprotein (NP), the stem region of hemagglutinin (HA), matrix proteins 1 and 2 (M1 and M2), the viral polymerase basic protein 1 (PB1), or the HA stem fused to a quadrivalent matrix protein 2 extracellular domain (M2e). Immunized mice were challenged with lethal doses of H5N1, H7N1 or H9N2 virus and monitored for disease symptoms and weight loss. To investigate the influence of previous exposure to influenza virus on protective immune responses induced by conserved influenza proteins, mice were infected with pandemic H1N1 virus (H1N1pdm09) prior to immunization and subsequently challenged with H5N1 virus. Antibody and T cell responses were assessed by ELISA and flow cytometry, respectively. RESULTS: MVA vectors expressing NP alone, or co-expressed with other conserved influenza proteins, protected mice against lethal challenge with H5N1, H7N1 or H9N2 virus. Pre-exposure to H1N1pdm09 increased protective efficacy against lethal H5N1 challenge. None of the other conserved influenza proteins provided significant levels of protection against lethal challenge. NP-expressing vectors induced high numbers of influenza-specific CD4(+) and CD8(+) T cells and high titer influenza-specific antibody responses. Higher influenza-specific CD4(+) T cell responses and NP-specific CD8(+) T cell responses were associated with increased protective efficacy. CONCLUSIONS: MVA vectors expressing influenza NP protect mice against lethal challenge with H5N1, H7N1 and H9N2 viruses by a mechanism involving influenza-specific CD4(+) and CD8(+) T cell responses.

Published

2014

7. Evaluation of OspA vaccination-induced serological correlates of protection against Lyme borreliosis in a mouse model.

Author

Michael G Schwendinger, Maria O'Rourke, Andreas Traweger, Helga Savidis-Dacho, Andreas Pilz, Daniel Portsmouth, Ian Livey, P Noel Barrett, and Brian A Crowe

Subjects

Medicine, Science

Abstract

For clinical development of a novel multivalent OspA vaccine against Lyme borreliosis, serological assays are required which can be used to establish immune correlates of protection against infection with Borrelia.Four assays (an OspA IgG ELISA, a competitive inhibition (CI) ELISA, a Borrelia surface-binding (SB) assay and a Borrelia killing assay) were used to evaluate the correlation between immune responses induced by rOspA 1/2 (a chimeric immunogen containing protective epitopes from OspA serotypes 1 and 2), and protective immunity against infection by B. burgdorferi s.s. (OspA-1) and B. afzelii (OspA-2). Mice were immunized with OspA 1/2 doses ranging from 0.3 ng to 100 ng, to induce a range of OspA antibody titers, and exposed to needle challenge with B. burgdorferi s.s. or tick challenge with B. afzelii. Receiver operator characteristics (ROC) curves were constructed for each assay, and the area under the curve (AUC), sensitivity, specificity and Youden Index were calculated. Potential cutoff antibody titers which could be used as correlates of vaccine-induced protection were derived from the maximum Youden Index.Immunization with OspA-1/2 provided dose-dependent protection against infection with B. burgdorferi s.s. and B. afzelii. Antibody responses detected by all four assays were highly significantly correlated with protection from infection by either B. burgdorferi s.s. (p

Published

2013

8. Pre-clinical efficacy and safety of experimental vaccines based on non-replicating vaccinia vectors against yellow fever.

Author

Birgit Schäfer, Georg W Holzer, Alexandra Joachimsthaler, Sogue Coulibaly, Michael Schwendinger, Brian A Crowe, Thomas R Kreil, P Noel Barrett, and Falko G Falkner

Subjects

Medicine, Science

Abstract

BACKGROUND: Currently existing yellow fever (YF) vaccines are based on the live attenuated yellow fever virus 17D strain (YFV-17D). Although, a good safety profile was historically attributed to the 17D vaccine, serious adverse events have been reported, making the development of a safer, more modern vaccine desirable. METHODOLOGY/PRINCIPAL FINDINGS: A gene encoding the precursor of the membrane and envelope (prME) protein of the YFV-17D strain was inserted into the non-replicating modified vaccinia virus Ankara and into the D4R-defective vaccinia virus. Candidate vaccines based on the recombinant vaccinia viruses were assessed for immunogenicity and protection in a mouse model and compared to the commercial YFV-17D vaccine. The recombinant live vaccines induced γ-interferon-secreting CD4- and functionally active CD8-T cells, and conferred full protection against lethal challenge already after a single low immunization dose of 10(5) TCID(50). Surprisingly, pre-existing immunity against wild-type vaccinia virus did not negatively influence protection. Unlike the classical 17D vaccine, the vaccinia virus-based vaccines did not cause mortality following intracerebral administration in mice, demonstrating better safety profiles. CONCLUSIONS/SIGNIFICANCE: The non-replicating recombinant YF candidate live vaccines induced a broad immune response after single dose administration, were effective even in the presence of a pre-existing immunity against vaccinia virus and demonstrated an excellent safety profile in mice.

Published

2011

9. Vectors based on modified vaccinia Ankara expressing influenza H5N1 hemagglutinin induce substantial cross-clade protective immunity.

Author

Annett Hessel, Michael Schwendinger, Georg W Holzer, Klaus K Orlinger, Sogue Coulibaly, Helga Savidis-Dacho, Marie-Luise Zips, Brian A Crowe, Thomas R Kreil, Hartmut J Ehrlich, P Noel Barrett, and Falko G Falkner

Subjects

Medicine, Science

Abstract

BACKGROUND: New highly pathogenic H5N1 influenza viruses are continuing to evolve with a potential threat for an influenza pandemic. So far, the H5N1 influenza viruses have not widely circulated in humans and therefore constitute a high risk for the non immune population. The aim of this study was to evaluate the cross-protective potential of the hemagglutinins of five H5N1 strains of divergent clades using a live attenuated modified vaccinia Ankara (MVA) vector vaccine. METHODOLOGY/PRINCIPAL FINDINGS: The replication-deficient MVA virus was used to express influenza hemagglutinin (HA) proteins. Specifically, recombinant MVA viruses expressing the HA genes of the clade 1 virus A/Vietnam/1203/2004 (VN/1203), the clade 2.1.3 virus A/Indonesia/5/2005 (IN5/05), the clade 2.2 viruses A/turkey/Turkey/1/2005 (TT01/05) and A/chicken/Egypt/3/2006 (CE/06), and the clade 2.3.4 virus A/Anhui/1/2005 (AH1/05) were constructed. These experimental live vaccines were assessed in a lethal mouse model. Mice vaccinated with the VN/1203 hemagglutinin-expressing MVA induced excellent protection against all the above mentioned clades. Also mice vaccinated with the IN5/05 HA expressing MVA induced substantial protection against homologous and heterologous AH1/05 challenge. After vaccination with the CE/06 HA expressing MVA, mice were fully protected against clade 2.2 challenge and partially protected against challenge of other clades. Mice vaccinated with AH1/05 HA expressing MVA vectors were only partially protected against homologous and heterologous challenge. The live vaccines induced substantial amounts of neutralizing antibodies, mainly directed against the homologous challenge virus, and high levels of HA-specific IFN-γ secreting CD4 and CD8 T-cells against epitopes conserved among the H5 clades and subclades. CONCLUSIONS/SIGNIFICANCE: The highest level of cross-protection was induced by the HA derived from the VN/1203 strain, suggesting that pandemic H5 vaccines utilizing MVA vector technology, should be based on the VN/1203 hemagglutinin. Furthermore, the recombinant MVA-HA-VN, as characterized in the present study, would be a promising candidate for such a vaccine.

Published

2011

10. A whole virus pandemic influenza H1N1 vaccine is highly immunogenic and protective in active immunization and passive protection mouse models.

Author

Otfried Kistner, Brian A Crowe, Walter Wodal, Astrid Kerschbaum, Helga Savidis-Dacho, Nicolas Sabarth, Falko G Falkner, Ines Mayerhofer, Wolfgang Mundt, Manfred Reiter, Leopold Grillberger, Christa Tauer, Michael Graninger, Alois Sachslehner, Michael Schwendinger, Peter Brühl, Thomas R Kreil, Hartmut J Ehrlich, and P Noel Barrett

Subjects

Medicine, Science

Abstract

The recent emergence and rapid spread of a novel swine-derived H1N1 influenza virus has resulted in the first influenza pandemic of this century. Monovalent vaccines have undergone preclinical and clinical development prior to initiation of mass immunization campaigns. We have carried out a series of immunogenicity and protection studies following active immunization of mice, which indicate that a whole virus, nonadjuvanted vaccine is immunogenic at low doses and protects against live virus challenge. The immunogenicity in this model was comparable to that of a whole virus H5N1 vaccine, which had previously been demonstrated to induce high levels of seroprotection in clinical studies. The efficacy of the H1N1 pandemic vaccine in protecting against live virus challenge was also seen to be equivalent to that of the H5N1 vaccine. The protective efficacy of the H1N1 vaccine was also confirmed using a severe combined immunodeficient (SCID) mouse model. It was demonstrated that mouse and guinea pig immune sera elicited following active H1N1 vaccination resulted in 100% protection of SCID mice following passive transfer of immune sera and lethal challenge. The immune responses to a whole virus pandemic H1N1 and a split seasonal H1N1 vaccine were also compared in this study. It was demonstrated that the whole virus vaccine induced a balanced Th-1 and Th-2 response in mice, whereas the split vaccine induced mainly a Th-2 response and only minimal levels of Th-1 responses. These data supported the initiation of clinical studies with the same low doses of whole virus vaccine that had previously been demonstrated to be immunogenic in clinical studies with a whole virus H5N1 vaccine.

Published

2010

11. A pandemic influenza H1N1 live vaccine based on modified vaccinia Ankara is highly immunogenic and protects mice in active and passive immunizations.

Author

Annett Hessel, Michael Schwendinger, Daniela Fritz, Sogue Coulibaly, Georg W Holzer, Nicolas Sabarth, Otfried Kistner, Walter Wodal, Astrid Kerschbaum, Helga Savidis-Dacho, Brian A Crowe, Thomas R Kreil, P Noel Barrett, and Falko G Falkner

Subjects

Medicine, Science

Abstract

BACKGROUND: The development of novel influenza vaccines inducing a broad immune response is an important objective. The aim of this study was to evaluate live vaccines which induce both strong humoral and cell-mediated immune responses against the novel human pandemic H1N1 influenza virus, and to show protection in a lethal animal challenge model. METHODOLOGY/PRINCIPAL FINDINGS: For this purpose, the hemagglutinin (HA) and neuraminidase (NA) genes of the influenza A/California/07/2009 (H1N1) strain (CA/07) were inserted into the replication-deficient modified vaccinia Ankara (MVA) virus--a safe poxviral live vector--resulting in MVA-H1-Ca and MVA-N1-Ca vectors. These live vaccines, together with an inactivated whole virus vaccine, were assessed in a lung infection model using immune competent Balb/c mice, and in a lethal challenge model using severe combined immunodeficient (SCID) mice after passive serum transfer from immunized mice. Balb/c mice vaccinated with the MVA-H1-Ca virus or the inactivated vaccine were fully protected from lung infection after challenge with the influenza H1N1 wild-type strain, while the neuraminidase virus MVA-N1-Ca induced only partial protection. The live vaccines were already protective after a single dose and induced substantial amounts of neutralizing antibodies and of interferon-gamma-secreting (IFN-gamma) CD4- and CD8 T-cells in lungs and spleens. In the lungs, a rapid increase of HA-specific CD4- and CD8 T cells was observed in vaccinated mice shortly after challenge with influenza swine flu virus, which probably contributes to the strong inhibition of pulmonary viral replication observed. In addition, passive transfer of antisera raised in MVA-H1-Ca vaccinated immune-competent mice protected SCID mice from lethal challenge with the CA/07 wild-type virus. CONCLUSIONS/SIGNIFICANCE: The non-replicating MVA-based H1N1 live vaccines induce a broad protective immune response and are promising vaccine candidates for pandemic influenza.

Published

2010

12. International Public Lending and American Policy

Author

Brian G. Crowe

Published

2019

13. Laboratory diagnosis of Lyme neuroborreliosis is influenced by the test used: Comparison of two ELISAs, immunoblot and CXCL13 testing

Author

Nora Wutte, Elisabeth Aberer, Elisabeth Daghofer, Brian A. Crowe, Werner Zenz, Franz Fazekas, and Juan J. Archelos

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Enzyme-Linked Immunosorbent Assay, Intrathecal, Sensitivity and Specificity, Gastroenterology, Diagnosis, Differential, Young Adult, Predictive Value of Tests, Borrelia, Internal medicine, Humans, Lyme Neuroborreliosis, Medicine, CXCL13, Child, Aged, biology, business.industry, Middle Aged, biology.organism_classification, medicine.disease, Chemokine CXCL13, Neurology, Borrelia burgdorferi, biology.protein, Female, Neurology (clinical), Antibody, business, Neuroborreliosis

Abstract

Purpose To compare Borrelia -specific intrathecal antibodies by two different ELISAs, an immunoblot (IB) and CXCL13. Methods Twenty-seven adults and 23 children with clinical symptoms compatible with NB were tested for Borrelia -specific intrathecal antibodies by flagellum ELISA-AI (flELISA), a recombinant ELISA-AI (rELISA) and by IB. Patients were classified according to the European Federation of Neurological Societies (EFNS) criteria as definite NB, possible NB, or non-NB. CSF CXCL13 levels were measured by ELISA. Results Among 50 patients, definite NB was diagnosed with the rELISA-AI in 29 (58%) patients, confirmed by IB in 19/29 patients, with flELISA-AI in 17 (34%) patients, confirmed by IB in 15/17 patients, and with IB in 20 (40%) patients. CXCL13 was positive in 22 (44%) patients. In 4 of 8 patients with negative AI, IB showed many detectable bands both in the CSF and serum. Conclusions The diagnosis of NB strongly relies on the used test method. The rELISA-AI test appears to be the most sensitive while the flELISA-AI is the least sensitive. However when the ELISA-AIs were confirmed by IB, different patients were identified as NB, while only 26% were identified by all performed test methods. There is a demand for standardized test methods with well-defined sensitivity and specificity to establish validated diagnostic criteria for NB including the use of the IB assay and CXCL13 as an additional non- Borrelia specific determinant in early NB.

Published

2014

14. A Novel Multivalent OspA Vaccine against Lyme Borreliosis Is Safe and Immunogenic in an Adult Population Previously Infected with Borrelia burgdorferi Sensu Lato

Author

Brian A. Crowe, Roland Weisser, Herwig Kollaritsch, Peter G. Kremsner, Ian Livey, Markus Zeitlinger, Eva-Maria Pöllabauer, Tomas Jelinek, Daniel Portsmouth, Maria O'Rourke, Bernhard Schmitt, R. Aschoff, Thomas Dvorak, Gerald Aichinger, Meral Esen, Ingomar Naudts, P. Noel Barrett, Michael G. Schwendinger, and Nina Wressnigg

Subjects

Adult, Male, Microbiology (medical), Serotype, Adolescent, Drug-Related Side Effects and Adverse Reactions, Lipoproteins, Clinical Biochemistry, Immunology, Population, Enzyme-Linked Immunosorbent Assay, Biology, complex mixtures, Young Adult, Lyme disease, Adjuvants, Immunologic, Borrelia burgdorferi Group, Double-Blind Method, Antigen, medicine, Humans, Immunology and Allergy, Borrelia burgdorferi, education, Aged, Lyme Disease, Vaccines, education.field_of_study, Immunogenicity, Vaccination, Middle Aged, bacterial infections and mycoses, medicine.disease, biology.organism_classification, Antibodies, Bacterial, Virology, Bacterial vaccine, Antigens, Surface, Bacterial Vaccines, bacteria, Alum Compounds, Female, Bacterial Outer Membrane Proteins

Abstract

Lyme borreliosis (LB) patients who recover, as well as previously infected asymptomatic individuals, remain vulnerable to reinfection withBorrelia burgdorferisensu lato. There is limited information available about the use of OspA vaccines in this population. In this study, a randomized double-blind phase I/II trial was performed to investigate the safety and immunogenicity of a novel multivalent OspA vaccine in healthy adults who were either seronegative or seropositive for previousB. burgdorferi sensu latoinfection. The participants received three monthly priming immunizations with either 30 μg or 60 μg alum-adjuvanted OspA antigen and a booster vaccination either 6 months or 9 to 12 months after the first immunization. The antibody responses to the six OspA serotypes included in the vaccine were evaluated. Adverse events were predominantly mild and transient and were similar in the seronegative and seropositive populations. Substantial enzyme-linked immunosorbent assay (ELISA) and surface-binding antibody responses against all six OspA antigens were induced after the primary immunization schedule in both populations, and they were substantially increased with both booster schedules. The antibody responses induced by the two doses were similar in the seronegative population, but there was a significant dose response in the seropositive population. These data indicate that the novel multivalent OspA vaccine is well tolerated and immunogenic in individuals previously infected withB. burgdorferi sensu lato. (This study is registered at ClinicalTrials.gov under registration no. NCT01504347.)

Published

2014

15. Safety and Immunogenicity of a Vero Cell Culture-Derived Whole-Virus H5N1 Influenza Vaccine in Chronically Ill and Immunocompromised Patients

Author

Richard Fritz, Wolfgang Herr, Thomas Dvorak, P. Noel Barrett, Christoph Stephan, Markus Zeitlinger, Eva Distler, Robert Sauermann, Hartmut J. Ehrlich, Gerald Aichinger, Brian A. Crowe, Alexander Geisberger, Daniel Portsmouth, Eva Wagner, and Maikel V. W. van der Velden

Subjects

Male, Microbiology (medical), H5N1 vaccine, Influenza vaccine, T-Lymphocytes, Clinical Biochemistry, Immunology, Immunization, Secondary, Cross Reactions, Antibodies, Viral, Lymphocyte Activation, medicine.disease_cause, Cell Line, Immunocompromised Host, Influenza A Virus, H1N1 Subtype, Chlorocebus aethiops, Influenza, Human, Influenza A virus, medicine, Animals, Humans, Immunology and Allergy, Neutralizing antibody, Vero Cells, Vaccines, Influenza A Virus, H5N1 Subtype, biology, Influenza A Virus, H3N2 Subtype, Immunogenicity, Vaccination, virus diseases, Hemagglutination Inhibition Tests, Middle Aged, Antibodies, Neutralizing, Virology, Influenza A virus subtype H5N1, Influenza B virus, Immunization, Influenza Vaccines, Antibody Formation, Chronic Disease, biology.protein, Female

Abstract

The development of vaccines against H5N1 influenza A viruses is a cornerstone of pandemic preparedness. Clinical trials of H5N1 vaccines have been undertaken in healthy subjects, but studies in risk groups have been lacking. In this study, the immunogenicity and safety of a nonadjuvanted cell culture-derived whole-virus H5N1 vaccine were assessed in chronically ill and immunocompromised adults. Subjects received two priming immunizations with a clade 1 A/Vietnam H5N1 influenza vaccine, and a subset also received a booster immunization with a clade 2.1 A/Indonesia H5N1 vaccine 12 to 24 months later. The antibody responses in the two populations were assessed by virus neutralization and single radial hemolysis assays. The T-cell responses in a subset of immunocompromised patients were assessed by enzyme-linked immunosorbent spot assay (ELISPOT). The priming and the booster vaccinations were safe and well tolerated in the two risk populations, and adverse reactions were predominantly mild and transient. The priming immunizations induced neutralizing antibody titers of ≥1:20 against the A/Vietnam strain in 64.2% of the chronically ill and 41.5% of the immunocompromised subjects. After the booster vaccination, neutralizing antibody titers of ≥1:20 against the A/Vietnam and A/Indonesia strains were achieved in 77.5% and 70.8%, respectively, of chronically ill subjects and in 71.6% and 67.5%, respectively, of immunocompromised subjects. The T-cell responses against the two H5N1 strains increased significantly over the baseline values. Substantial heterosubtypic T-cell responses were elicited against the 2009 pandemic H1N1 virus and seasonal A(H1N1), A(H3N2), and B subtypes. There was a significant correlation between T-cell responses and neutralizing antibody titers. These data indicate that nonadjuvanted whole-virus cell culture-derived H5N1 influenza vaccines are suitable for immunizing chronically ill and immunocompromised populations. (This study is registered at ClinicalTrials.gov under registration no. NCT00711295.)

Published

2014

16. Are Poor Sleepers Afraid of the Dark? A Preliminary Investigation

Author

Colleen E. Carney, Molly E. Atwood, Alex J. Andrews, Brian M. Crowe, and Taryn G. Moss

Subjects

Poor sleep, Psychiatry and Mental health, Clinical Psychology, genetic structures, Insomnia, medicine, Anxiety, sense organs, medicine.symptom, Psychology, Sleep in non-human animals, Clinical psychology

Abstract

No studies have investigated whether those with poor sleep are aware of being uncomfortable in the dark via subjective inquiry, and no study has evaluated whether poor sleepers have increased fear in the dark using objective indices (e.g., a validated startle paradigm). Good and poor sleepers (N = 108) completed questionnaires about their level of discomfort with the dark and were evaluated for an increased startle reflex by measuring eyeblink latency via electrooculogram in response to unexpected noise in the dark and the light. Participants listened to bursts of unexpected white noise, while in counterbalanced light/dark conditions. Relative to good sleepers, more poor sleepers reported increased discomfort in the dark. There was a significant lighting × time × sleeper status interaction for eyeblink latency. Relative to the first trial in the dark, eyeblink latency in good sleepers increased in the second dark exposure; suggesting habituation in the dark. Eyeblink latency in poor sleepers did not decrease. Thus, poor sleepers reported being uncomfortable in the dark and they remained more easily startled in the dark over the course of the study. It is unclear if the dark may predispose people to sleep problems, or if sleep problems sensitize poor sleepers to fear darkness.

Published

2013

17. Safety and immunogenicity of a novel multivalent OspA vaccine against Lyme borreliosis in healthy adults: a double-blind, randomised, dose-escalation phase 1/2 trial

Author

Andreas Pilz, Michael G. Schwendinger, Maria Paulke-Korinek, Meral Esen, Peter G. Kremsner, Eva-Maria Pöllabauer, Bernhard Schmitt, Ian Livey, Brian A. Crowe, Clair L. Firth, Sandor Fritsch, Nina Wressnigg, Hartmut J. Ehrlich, Daniel Portsmouth, Peter Brühl, Benjamin J. Luft, Thomas Dvorak, Alexandra Löw-Baselli, P. Noel Barrett, Markus Müller, Herwig Kollaritsch, Julia Singer, Gerald Aichinger, and Markus Zeitlinger

Subjects

Adult, Male, Serotype, Lipoproteins, medicine.medical_treatment, Pain, Young Adult, Lyme disease, Adjuvants, Immunologic, Double-Blind Method, medicine, Humans, Borrelia burgdorferi, Adverse effect, biology, business.industry, Immunogenicity, Headache, Lyme Disease Vaccines, Middle Aged, bacterial infections and mycoses, biology.organism_classification, medicine.disease, Vaccination, Infectious Diseases, Immunoglobulin G, Antigens, Surface, Bacterial Vaccines, Immunology, Female, Bacterial antigen, business, Adjuvant, Bacterial Outer Membrane Proteins

Abstract

Lyme borreliosis is caused by Borrelia burgdorferi sensu stricto in the USA and by several Borrelia species in Europe and Asia, but no human vaccine is available. We investigated the safety and immunogenicity of adjuvanted and non-adjuvanted vaccines containing protective epitopes from Borrelia species outer surface protein A (OspA) serotypes in healthy adults.Between March 1, 2011, and May 8, 2012, we did a double-blind, randomised, dose-escalation phase 1/2 study at four sites in Austria and Germany. Healthy adults aged 18-70 years who were seronegative for B. burgdorferi sensu lato were eligible for inclusion. Participants were recruited sequentially and randomly assigned to one of six study groups in equal ratios via an electronic data capture system. Participants and investigators were masked to group allocation. Participants received three vaccinations containing 30 μg, 60 μg, or 90 μg OspA antigen with or without an adjuvant, with intervals of 28 days, and a booster 9-12 months after the first immunisation. The coprimary endpoints were the frequency and severity of injection-site and systemic reactions within 7 days of each vaccination, and the antibody responses to OspA serotypes 1-6, as established by ELISA. This study is registered with ClinicalTrials.gov, number NCT01504347.300 participants were randomly assigned: 151 to adjuvanted vaccines (50 to 30 μg, 51 to 60 μg, and 50 to 90 μg doses), and 149 to non-adjuvanted vaccines (50 to 30 μg, 49 to 60 μg, and 50 to 90 μg doses). Adverse reactions were predominantly mild, and no vaccine-related serious adverse events were reported. The risk of systemic reactions (risk ratio 0·54 [95% CI 0·41-0·70]; p0·0001) and of moderate or severe systemic reactions (0·35 [0·13-0·92]; p=0·034) was significantly lower for adjuvanted than non-adjuvanted formulations. The 30 μg adjuvanted formulation had the best tolerability profile; only headache (five [10%, 95% CI 4-20] of 50), injection-site pain (16 [32%, 21-45]), and tenderness (17 [34%, 23-47]) affected more than 6% of patients. All doses and formulations induced substantial mean IgG antibody titres against OspA serotypes 1-6 after the first three vaccinations (range 6944-17,321) and booster (19,056-32,824) immunisations. The 30 μg adjuvanted formulation induced the highest antibody titres after the booster: range 26,143 (95% CI 18,906-36,151) to 42,381 (31,288-57,407).The novel multivalent OspA vaccine could be an effective intervention for prevention of Lyme borreliosis in Europe and the USA, and possibly worldwide. Larger confirmatory formulation studies will need to be done that include individuals seropositive for Borrelia burgdorferi sensu lato before placebo-controlled phase 3 efficacy studies can begin.Baxter.

Published

2013

18. A cell culture-derived whole-virus H5N1 vaccine induces long-lasting cross-clade protective immunity in mice which is augmented by a homologous or heterologous booster vaccination

Author

Brian A. Crowe, Nicolas Sabarth, Daniel Portsmouth, Helga Savidis-Dacho, Michael G. Schwendinger, P. Noel Barrett, M. Keith Howard, Thomas R. Kreil, Otfried Kistner, and Peter Brühl

Subjects

H5N1 vaccine, Influenza vaccine, animal diseases, Population, Dose-Response Relationship, Immunologic, Immunization, Secondary, Antibodies, Heterophile, chemical and pharmacologic phenomena, Booster dose, Cross Reactions, Biology, Mice, Immunity, Chlorocebus aethiops, Animals, education, Vero Cells, Immunization Schedule, Duck embryo vaccine, Immunity, Cellular, education.field_of_study, Heterologous vaccine, Influenza A Virus, H5N1 Subtype, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, biochemical phenomena, metabolism, and nutrition, Antibodies, Neutralizing, Virology, Immunity, Humoral, Vaccination, Infectious Diseases, Influenza Vaccines, Immunology, bacteria, Molecular Medicine, Female

Abstract

Background Preparation for an H5N1 influenza pandemic in humans could include priming the population in the pre-pandemic period with a vaccine produced from an existing H5N1 vaccine strain, with the possibility of boosting with a pandemic virus vaccine when it becomes available. We investigated the longevity of the immune response after one or two priming immunizations with a whole-virus H5N1 vaccine and the extent to which this can be boosted by later immunization with either a homologous or heterologous vaccine. Methods Mice received one or two priming immunizations with a Vero cell culture-derived, whole-virus clade 1 H5N1 vaccine formulated to contain either 750 ng or 30 ng hemagglutinin. Six months after the first priming immunization, mice received either a booster immunization with the same clade 1 vaccine or a heterologous clade 2.1 vaccine, or buffer. Humoral and cellular immune responses were evaluated before and at regular intervals after immunizations. Three weeks after booster immunization, mice were challenged with a lethal dose of wild-type H5N1 virus from clades 1, 2.1 or 2.2 and survival was monitored for 14 days. Results One or two priming immunizations with the 750 ng or 30 ng HA formulations, respectively, induced H5N1-neutralizing antibody titers which were maintained for ≥6 months and provided long-term cross-clade protection against wild-type virus challenge. Both humoral and cellular immune responses were substantially increased by a booster immunization after 6 months. The broadest protective immunity was provided by an immunization regimen consisting of one or two priming immunizations with a clade 1 vaccine and a boosting immunization with a clade 2.1 vaccine. Conclusions These data support the concept that pre-pandemic vaccination can provide robust and long-lasting H5N1 immunity which could be effectively boosted by immunization either with another pre-pandemic vaccine or with the pandemic strain vaccine.

Published

2012

19. GATA-1, G208S macrothrombocytes are deficient in talin: Immunofluorescence studies

Author

James G. White, Brian R Crowe, and Steven M. Burris

Subjects

Blood Platelets, Talin, macromolecular substances, In Vitro Techniques, Immunofluorescence, Ultrastructural Pathology, Cell membrane, Western blot, medicine, Humans, GATA1 Transcription Factor, Actin-binding protein, Cytoskeleton, Polyacrylamide gel electrophoresis, biology, medicine.diagnostic_test, Cell Membrane, Genetic Diseases, X-Linked, Hematology, General Medicine, Molecular biology, medicine.anatomical_structure, Mutation, embryonic structures, biology.protein, Cytochemistry

Abstract

Previous investigations from our laboratory identified the ultrastructural pathology and cytochemistry of macrothrombocytes (MTC) from patients with the X-linked, G208S varient of the GATA-1 mutation.A subsequent biochemical study of the MTC cytoskeletal proteins using polyacrylamide gel electrophoresis and western blot analysis revealed the MTC were deficient in the high-molecular weight, actin binding protein, talin. The present study has used immunofluorescent techniques to further characterize the talin deficiency. Results confirm that the GATA-1, G208S MTC are deficient in talin, and what little is present relocates to the undersurface of the plasma membrane following activations where it associates with adhesion plaques.

Published

2009

20. Immunogenicity and Protective Efficacy of a Vero Cell Culture-Derived Whole-Virus H7N9 Vaccine in Mice and Guinea Pigs

Author

Dalida Balta, Walter Wodal, Anita Karner-Pichl, Otfried Kistner, Brian A. Crowe, Peter Brühl, Helga Savidis-Dacho, Leopold Grillberger, M. Keith Howard, Richard Fritz, P. Noel Barrett, Michael G. Schwendinger, Daniel Portsmouth, and Christine Hohenadl

Subjects

viruses, Science, Guinea Pigs, Neuraminidase, Hemagglutinin Glycoproteins, Influenza Virus, medicine.disease_cause, Antibodies, Viral, Influenza A Virus, H7N9 Subtype, Virus, Interferon-gamma, Mice, Immune system, Influenza A Virus, H1N1 Subtype, Th2 Cells, Orthomyxoviridae Infections, Chlorocebus aethiops, Influenza A virus, medicine, Animals, Vero Cells, Multidisciplinary, biology, Viral Vaccine, Immunogenicity, Hemagglutination Inhibition Tests, Th1 Cells, Virology, Influenza Vaccines, Mice, Inbred DBA, Immunoglobulin G, Antibody Formation, biology.protein, Vero cell, Medicine, Female, Interleukin-4, Antibody, Research Article

Abstract

BackgroundA novel avian H7N9 virus with a high case fatality rate in humans emerged in China in 2013. We evaluated the immunogenicity and protective efficacy of a candidate Vero cell culture-derived whole-virus H7N9 vaccine in small animal models.MethodsAntibody responses induced in immunized DBA/2J mice and guinea pigs were evaluated by hemagglutination inhibition (HI), microneutralization (MN), and neuraminidase inhibition (NAi) assays. T-helper cell responses and IgG subclass responses in mice were analyzed by ELISPOT and ELISA, respectively. Vaccine efficacy against lethal challenge with wild-type H7N9 virus was evaluated in immunized mice. H7N9-specific antibody responses induced in mice and guinea pigs were compared to those induced by a licensed whole-virus pandemic H1N1 (H1N1pdm09) vaccine.ResultsThe whole-virus H7N9 vaccine induced dose-dependent H7N9-specific HI, MN and NAi antibodies in mice and guinea pigs. Evaluation of T-helper cell responses and IgG subclasses indicated the induction of a balanced Th1/Th2 response. Immunized mice were protected against lethal H7N9 challenge in a dose-dependent manner. H7N9 and H1N1pdm09 vaccines were similarly immunogenic.ConclusionsThe induction of H7N9-specific antibody and T cell responses and protection against lethal challenge suggest that the Vero cell culture-derived whole-virus vaccine would provide an effective intervention against the H7N9 virus.

Published

2015

21. A double-inactivated whole virus candidate SARS coronavirus vaccine stimulates neutralising and protective antibody responses

Author

Martin Spruth, Manfred Reiter, Wolfgang Mundt, Otfried Kistner, Peter Brühl, Helga Savidis-Dacho, Christa Tauer, Leopold Grillberger, P. Noel Barrett, Brian A. Crowe, Elisabeth Hitter, and Marijan Gerencer

Subjects

SARS coronavirus, Double-inactivated vaccine, medicine.medical_treatment, viruses, Blotting, Western, Dose-Response Relationship, Immunologic, Enzyme-Linked Immunosorbent Assay, medicine.disease_cause, Antibodies, Viral, Severe Acute Respiratory Syndrome, Virus, Article, Microbiology, Neutralisation, Tissue Culture Techniques, Mice, Adjuvants, Immunologic, Neutralization Tests, Chlorocebus aethiops, medicine, Animals, Vero Cells, Coronavirus, Mice, Inbred BALB C, Protection, General Veterinary, General Immunology and Microbiology, biology, Immunogenicity, Public Health, Environmental and Occupational Health, Viral Vaccines, Virology, Vaccination, Infectious Diseases, Severe acute respiratory syndrome-related coronavirus, Vaccines, Inactivated, Humoral immunity, Fermentation, biology.protein, Vero cell, Molecular Medicine, Electrophoresis, Polyacrylamide Gel, Female, Immunization, Antibody, Adjuvant

Abstract

A double-inactivated, candidate whole virus vaccine against severe acute respiratory syndrome associated coronavirus (SARS-CoV) was developed and manufactured at large scale using fermenter cultures of serum protein free Vero cells. A two step inactivation procedure involving sequential formaldehyde and U.V. inactivation was utilised in order to ensure an extremely high safety margin with respect to residual infectivity. The immunogenicity of this double-inactivated vaccine was characterised in the mouse model. Mice that were immunised twice with the candidate SARS-CoV vaccine developed high antibody titres against the SARS-CoV spike protein and high levels of neutralising antibodies. The use of the adjuvant Al(OH)3 had only a minor effect on the immunogenicity of the vaccine. In addition, cell mediated immunity as measured by interferon-gamma and interleukin-4 stimulation, was elicited by vaccination. Moreover, the vaccine confers protective immunity as demonstrated by prevention of SARS-CoV replication in the respiratory tract of mice after intranasal challenge with SARS-CoV. Protection of mice was correlated to antibody titre against the SARS-CoV S protein and neutralising antibody titre.

Published

2005

22. MVA Vectors Expressing Conserved Influenza Proteins Protect Mice against Lethal Challenge with H5N1, H9N2 and H7N1 Viruses

Author

Brian A. Crowe, Annett Hessel, P. Noel Barrett, Birgit Schäfer, Thomas R. Kreil, Sogue Coulibaly, Andreas Pilz, Michael G. Schwendinger, Daniel Portsmouth, Helga Savidis-Dacho, and Falko G. Falkner

Subjects

Viral Diseases, viruses, T-Lymphocytes, lcsh:Medicine, medicine.disease_cause, chemistry.chemical_compound, Mice, Influenza A Virus, H9N2 Subtype, Cytotoxic T cell, lcsh:Science, Mice, Inbred BALB C, Multidisciplinary, biology, T Cells, Vaccination, virus diseases, Infectious Diseases, Influenza Vaccines, Medicine, Influenza A Virus, H7N1 Subtype, Female, Antibody, Research Article, Influenza vaccine, Immune Cells, Immunology, Enzyme-Linked Immunosorbent Assay, Vaccinia virus, Microbiology, Virus, Immune system, Orthomyxoviridae Infections, Virology, Vaccine Development, medicine, Animals, Biology, Influenza A Virus, H5N1 Subtype, lcsh:R, Immunity, Viral Vaccines, Influenza A virus subtype H5N1, Influenza, chemistry, biology.protein, lcsh:Q, Clinical Immunology, Vaccinia

Abstract

BACKGROUND: The availability of a universal influenza vaccine able to induce broad cross-reactive immune responses against diverse influenza viruses would provide an alternative to currently available strain-specific vaccines. We evaluated the ability of vectors based on modified vaccinia virus Ankara (MVA) expressing conserved influenza proteins to protect mice against lethal challenge with multiple influenza subtypes. METHODS: Mice were immunized with MVA vectors expressing H5N1-derived nucleoprotein (NP), the stem region of hemagglutinin (HA), matrix proteins 1 and 2 (M1 and M2), the viral polymerase basic protein 1 (PB1), or the HA stem fused to a quadrivalent matrix protein 2 extracellular domain (M2e). Immunized mice were challenged with lethal doses of H5N1, H7N1 or H9N2 virus and monitored for disease symptoms and weight loss. To investigate the influence of previous exposure to influenza virus on protective immune responses induced by conserved influenza proteins, mice were infected with pandemic H1N1 virus (H1N1pdm09) prior to immunization and subsequently challenged with H5N1 virus. Antibody and T cell responses were assessed by ELISA and flow cytometry, respectively. RESULTS: MVA vectors expressing NP alone, or co-expressed with other conserved influenza proteins, protected mice against lethal challenge with H5N1, H7N1 or H9N2 virus. Pre-exposure to H1N1pdm09 increased protective efficacy against lethal H5N1 challenge. None of the other conserved influenza proteins provided significant levels of protection against lethal challenge. NP-expressing vectors induced high numbers of influenza-specific CD4(+) and CD8(+) T cells and high titer influenza-specific antibody responses. Higher influenza-specific CD4(+) T cell responses and NP-specific CD8(+) T cell responses were associated with increased protective efficacy. CONCLUSIONS: MVA vectors expressing influenza NP protect mice against lethal challenge with H5N1, H7N1 and H9N2 viruses by a mechanism involving influenza-specific CD4(+) and CD8(+) T cell responses.

Published

2014

23. Guest Editorial – Some Reflections on the Common Foreign and Security Policy

Author

Brian L. Crowe

Published

1998

24. Evaluation of OspA vaccination-induced serological correlates of protection against Lyme borreliosis in a mouse model

Author

Maria O'Rourke, Helga Savidis-Dacho, P. Noel Barrett, Andreas Pilz, Ian Livey, Michael G. Schwendinger, Daniel Portsmouth, Andreas Traweger, and Brian A. Crowe

Subjects

Immunogen, Lipoproteins, Dose-Response Relationship, Immunologic, lcsh:Medicine, complex mixtures, Serology, Mice, Lyme disease, Antigen, Borrelia, medicine, Animals, Borrelia burgdorferi, lcsh:Science, Lyme Disease, Multidisciplinary, biology, lcsh:R, Vaccination, Antibody titer, Lyme Disease Vaccines, medicine.disease, biology.organism_classification, bacterial infections and mycoses, Virology, Antibodies, Bacterial, Disease Models, Animal, Immunoglobulin G, Immunology, Antigens, Surface, Bacterial Vaccines, biology.protein, bacteria, lcsh:Q, Female, Antibody, Bacterial Outer Membrane Proteins, Research Article

Abstract

Background For clinical development of a novel multivalent OspA vaccine against Lyme borreliosis, serological assays are required which can be used to establish immune correlates of protection against infection with Borrelia. Methods Four assays (an OspA IgG ELISA, a competitive inhibition (CI) ELISA, a Borrelia surface-binding (SB) assay and a Borrelia killing assay) were used to evaluate the correlation between immune responses induced by rOspA 1/2 (a chimeric immunogen containing protective epitopes from OspA serotypes 1 and 2), and protective immunity against infection by B. burgdorferi s.s. (OspA-1) and B. afzelii (OspA-2). Mice were immunized with OspA 1/2 doses ranging from 0.3 ng to 100 ng, to induce a range of OspA antibody titers, and exposed to needle challenge with B. burgdorferi s.s. or tick challenge with B. afzelii. Receiver operator characteristics (ROC) curves were constructed for each assay, and the area under the curve (AUC), sensitivity, specificity and Youden Index were calculated. Potential cutoff antibody titers which could be used as correlates of vaccine-induced protection were derived from the maximum Youden Index. Results Immunization with OspA-1/2 provided dose-dependent protection against infection with B. burgdorferi s.s. and B. afzelii. Antibody responses detected by all four assays were highly significantly correlated with protection from infection by either B. burgdorferi s.s. (p

Published

2013

25. Preclinical evaluation of Vaxfectin®-adjuvanted Vero cell-derived seasonal split and pandemic whole virus influenza vaccines

Author

Brian A. Crowe, Sean M. Sullivan, Mark Shlapobersky, Walter Wodal, Otfried Kistner, Jukka Hartikka, Helga Savidis-Dacho, Astrid Kerschbaum, Alain Rolland, Peter Dipl Biol Dr Bruehl, P. Noel Barrett, Michael G. Schwendinger, and Larry R. Smith

Subjects

Influenza vaccine, T-Lymphocytes, Immunology, Guinea Pigs, Biology, medicine.disease_cause, Antibodies, Viral, Virus, Microbiology, Interferon-gamma, Mice, Adjuvants, Immunologic, Influenza A virus, medicine, Immunology and Allergy, Animals, Pharmacology, Mice, Inbred BALB C, Hemagglutination assay, Immunogenicity, Phosphatidylethanolamines, Antibody titer, Hemagglutination Inhibition Tests, Virology, Influenza A virus subtype H5N1, Treatment Outcome, Influenza Vaccines, Vaccines, Subunit, Vero cell, Female, Research Paper

Abstract

Increasing the potency and supply of seasonal and pandemic influenza vaccines remains an important unmet medical need which may be effectively accomplished with adjuvanted egg- or cell culture-derived vaccines. Vaxfectin®, a cationic lipid-based adjuvant with a favorable safety profile in phase 1 plasmid DNA vaccines trials, was tested in combination with seasonal split, trivalent and pandemic whole virus, monovalent influenza vaccines produced in Vero cell cultures. Comparison of hemagglutination inhibition (HI) antibody titers in Vaxfectin®-adjuvanted to nonadjuvanted vaccinated mice and guinea pigs revealed 3- to 20-fold increases in antibody titers against each of the trivalent influenza virus vaccine strains and 2- to 8-fold increases in antibody titers against the monovalent H5N1 influenza virus vaccine strain. With the vaccine doses tested, comparable antibody responses were induced with formulations that were freshly prepared or refrigerated at conventional 2–8°C storage conditions for up to 6 mo. Comparison of T-cell frequencies measured by interferon-gamma ELISPOT assay between groups revealed increases of between 2- to 10-fold for each of the adjuvanted trivalent strains and up to 22-fold higher with monovalent H5N1 strain. Both trivalent and monovalent vaccines were easy to formulate with Vaxfectin® by simple mixing. These preclinical data support further testing of Vaxfectin®-adjuvanted Vero cell culture vaccines toward clinical studies designed to assess safety and immunogenicity of these vaccines in humans.

Published

2013

26. A new approach to a Lyme disease vaccine

Author

Benjamin J. Luft, Xiaohua Yang, P. Noel Barrett, Brian A. Crowe, Ian Livey, Maria O'Rourke, Helga Savidis-Dacho, John J. Dunn, and Andreas Traweger

Subjects

Microbiology (medical), medicine.medical_treatment, Lipoproteins, Borrelia afzelii, medicine.disease_cause, complex mixtures, Epitope, Microbiology, Epitopes, Mice, Lyme disease, Ticks, Antigen, Borrelia burgdorferi Group, Borrelia, parasitic diseases, medicine, Animals, Borrelia burgdorferi, Lyme Disease, Mice, Inbred C3H, biology, Lyme Disease Vaccines, bacterial infections and mycoses, biology.organism_classification, medicine.disease, Virology, Antibodies, Bacterial, Recombinant Proteins, Vaccination, Infectious Diseases, Antigens, Surface, Bacterial Vaccines, Models, Animal, bacteria, Adjuvant, Bacterial Outer Membrane Proteins

Abstract

A single recombinant outer surface protein A (OspA) antigen designed to contain protective elements from 2 different OspA serotypes (1 and 2) is able to induce antibody responses that protect mice against infection with either Borrelia burgdorferi sensu stricto (OspA serotype-1) or Borrelia afzelii (OspA serotype-2). Protection against infection with B burgdorferi ss strain ZS7 was demonstrated in a needle-challenge model. Protection against B. afzelii species was shown in a tick-challenge model using feral ticks. In both models, as little as .03 μg of antigen, when administered in a 2-dose immunization schedule with aluminum hydroxide as adjuvant, was sufficient to provide complete protection against the species targeted. This proof of principle study proves that knowledge of protective epitopes can be used for the rational design of effective, genetically modified vaccines requiring fewer OspA antigens and suggests that this approach may facilitate the development of an OspA vaccine for global use.

Published

2011

27. Foreign Policy‐Making: Reflections of a Practitioner

Author

Brian L. Crowe

Subjects

International relations, Public Administration, Sociology and Political Science, European community, Foreign Policy Making, Domestic policy, language.human_language, Danish, Political economy, Political science, Development economics, medicine, language, medicine.symptom, Collapse (medical)

Abstract

The Impact of Domestic Policy on International relations and vice versa has seldom been more clearly demonstrated than in late autumn 1992, with the near collapse in November of the Uruguay Round and the series of events in the European Community surrounding the Danish and French referenda and Britian's forced withdrawal from the ERM being only the two most glaring examples.

Published

1993

28. Lyme disease vaccination: safety first – Authors' reply

Author

Brian A. Crowe, P. Noel Barrett, Daniel Portsmouth, Gerald Aichinger, and Nina Wressnigg

Subjects

Male, Pediatrics, medicine.medical_specialty, business.industry, Lipoproteins, MEDLINE, Lyme Disease Vaccines, medicine.disease, Vaccination, Infectious Diseases, Lyme disease, Adjuvants, Immunologic, Borrelia burgdorferi, Antigens, Surface, Bacterial Vaccines, medicine, Humans, Safety first, Female, business, Bacterial Outer Membrane Proteins

Published

2014

29. Pre-clinical efficacy and safety of experimental vaccines based on non-replicating vaccinia vectors against yellow fever

Author

Birgit Schäfer, Brian A. Crowe, Thomas R. Kreil, Georg Holzer, Alexandra Joachimsthaler, Falko G. Falkner, Sogue Coulibaly, P. Noel Barrett, and Michael G. Schwendinger

Subjects

CD4-Positive T-Lymphocytes, Viral Diseases, viruses, lcsh:Medicine, Gene Expression, CD8-Positive T-Lymphocytes, chemistry.chemical_compound, Mice, Viral Envelope Proteins, Chlorocebus aethiops, Molecular Cell Biology, Clinical efficacy, lcsh:Science, Immune Response, Mice, Inbred BALB C, Multidisciplinary, Viral Vaccine, Yellow fever, Yellow Fever Vaccine, Infectious Diseases, Medicine, medicine.drug, Plasmids, Research Article, Immunology, Yellow fever vaccine, Vaccinia virus, Biology, Vaccines, Attenuated, Virus, Molecular Genetics, Immune system, Yellow Fever, medicine, Genetics, Animals, Humans, Adverse effect, Vero Cells, lcsh:R, Viral Vaccines, medicine.disease, Virology, chemistry, Immune System, lcsh:Q, Vaccinia, HeLa Cells

Abstract

BACKGROUND: Currently existing yellow fever (YF) vaccines are based on the live attenuated yellow fever virus 17D strain (YFV-17D). Although, a good safety profile was historically attributed to the 17D vaccine, serious adverse events have been reported, making the development of a safer, more modern vaccine desirable. METHODOLOGY/PRINCIPAL FINDINGS: A gene encoding the precursor of the membrane and envelope (prME) protein of the YFV-17D strain was inserted into the non-replicating modified vaccinia virus Ankara and into the D4R-defective vaccinia virus. Candidate vaccines based on the recombinant vaccinia viruses were assessed for immunogenicity and protection in a mouse model and compared to the commercial YFV-17D vaccine. The recombinant live vaccines induced γ-interferon-secreting CD4- and functionally active CD8-T cells, and conferred full protection against lethal challenge already after a single low immunization dose of 10(5) TCID(50). Surprisingly, pre-existing immunity against wild-type vaccinia virus did not negatively influence protection. Unlike the classical 17D vaccine, the vaccinia virus-based vaccines did not cause mortality following intracerebral administration in mice, demonstrating better safety profiles. CONCLUSIONS/SIGNIFICANCE: The non-replicating recombinant YF candidate live vaccines induced a broad immune response after single dose administration, were effective even in the presence of a pre-existing immunity against vaccinia virus and demonstrated an excellent safety profile in mice.

Published

2010

30. A Pandemic Influenza H1N1 Live Vaccine Based on Modified Vaccinia Ankara Is Highly Immunogenic and Protects Mice in Active and Passive Immunizations

Author

Helga Savidis-Dacho, Daniela Fritz, P. Noel Barrett, Brian A. Crowe, Nicolas Sabarth, Thomas R. Kreil, Walter Wodal, Annett Hessel, Michael G. Schwendinger, Sogue Coulibaly, Georg Holzer, Falko G. Falkner, Astrid Kerschbaum, and Otfried Kistner

Subjects

Modified vaccinia Ankara, viruses, lcsh:Medicine, Neuraminidase, Hemagglutinin Glycoproteins, Influenza Virus, CD8-Positive T-Lymphocytes, Cross Reactions, Vaccines, Attenuated, Virus, Cell Line, Disease Outbreaks, Mice, Immune system, Influenza A Virus, H1N1 Subtype, Antibody Specificity, Pandemic, Infectious Diseases/Viral Infections, Influenza, Human, Animals, Humans, lcsh:Science, Molecular Biology, Lung, Virology/Vaccines, Multidisciplinary, Attenuated vaccine, biology, Viral Vaccine, lcsh:R, Vaccination, Immunization, Passive, virus diseases, Virology, Influenza Vaccines, Immunology, Immunology/Immune Response, Antibody Formation, biology.protein, Virology/Animal Models of Infection, lcsh:Q, Female, Immunocompetence, Spleen, Research Article

Abstract

BACKGROUND: The development of novel influenza vaccines inducing a broad immune response is an important objective. The aim of this study was to evaluate live vaccines which induce both strong humoral and cell-mediated immune responses against the novel human pandemic H1N1 influenza virus, and to show protection in a lethal animal challenge model. METHODOLOGY/PRINCIPAL FINDINGS: For this purpose, the hemagglutinin (HA) and neuraminidase (NA) genes of the influenza A/California/07/2009 (H1N1) strain (CA/07) were inserted into the replication-deficient modified vaccinia Ankara (MVA) virus--a safe poxviral live vector--resulting in MVA-H1-Ca and MVA-N1-Ca vectors. These live vaccines, together with an inactivated whole virus vaccine, were assessed in a lung infection model using immune competent Balb/c mice, and in a lethal challenge model using severe combined immunodeficient (SCID) mice after passive serum transfer from immunized mice. Balb/c mice vaccinated with the MVA-H1-Ca virus or the inactivated vaccine were fully protected from lung infection after challenge with the influenza H1N1 wild-type strain, while the neuraminidase virus MVA-N1-Ca induced only partial protection. The live vaccines were already protective after a single dose and induced substantial amounts of neutralizing antibodies and of interferon-gamma-secreting (IFN-gamma) CD4- and CD8 T-cells in lungs and spleens. In the lungs, a rapid increase of HA-specific CD4- and CD8 T cells was observed in vaccinated mice shortly after challenge with influenza swine flu virus, which probably contributes to the strong inhibition of pulmonary viral replication observed. In addition, passive transfer of antisera raised in MVA-H1-Ca vaccinated immune-competent mice protected SCID mice from lethal challenge with the CA/07 wild-type virus. CONCLUSIONS/SIGNIFICANCE: The non-replicating MVA-based H1N1 live vaccines induce a broad protective immune response and are promising vaccine candidates for pandemic influenza.

Published

2010

31. Evaluation of the cellular immune responses induced by a non-adjuvanted inactivated whole virus A/H5N1/VN/1203 pandemic influenza vaccine in humans

Author

Andreas Pilz, Michael G. Schwendinger, Gerald Aichinger, Hartmut J. Ehrlich, Marijan Gerencer, Brian A. Crowe, Julia Singer, Markus Müller, Otfried Kistner, P. Noel Barrett, Markus Zeitlinger, Peter Brühl, and Katrin Koelling-Schlebusch

Subjects

Adult, CD4-Positive T-Lymphocytes, Cellular immunity, H5N1 vaccine, Adolescent, Influenza vaccine, viruses, animal diseases, T cell, Immunization, Secondary, Biology, Cross Reactions, medicine.disease_cause, Virus, Young Adult, Immune system, Influenza A Virus, H1N1 Subtype, Chlorocebus aethiops, Influenza, Human, medicine, Animals, Humans, Memory B cell, Pandemics, Vero Cells, Aged, Aged, 80 and over, B-Lymphocytes, Immunity, Cellular, General Veterinary, General Immunology and Microbiology, Influenza A Virus, H5N1 Subtype, Influenza A Virus, H3N2 Subtype, Vaccination, Public Health, Environmental and Occupational Health, virus diseases, Middle Aged, Virology, Influenza A virus subtype H5N1, Influenza B virus, Infectious Diseases, medicine.anatomical_structure, Vaccines, Inactivated, Influenza Vaccines, Immunology, Molecular Medicine, Immunologic Memory

Abstract

In the present study the homologous and heterologous type and subtype specific cellular immune response induced by a wild type inactivated whole virus H5N1 Influenza (A/Vietnam/1203/2004) vaccine was evaluated. Two immunizations with the Vero cell derived H5N1 influenza vaccine on Day 0 and Day 21 induced significant H5N1 vaccine specific and H5 haemagglutinin specific clade and cross-clade reactive CD4(+) T cell responses, which were maintained at significant levels for at least 6 months. The H5N1 vaccine specific response cross-reacted with the H1N1, but not with H3N2 or B seasonal Influenza strains. The vaccine significantly increased the number of H5N1 specific and H5 haemagglutinin specific memory B cells, 6 months after the primary immunization, however no H1N1 specific cross-reactivity was observed. Importantly, the inactivated whole virus H5N1 vaccine was just as effective in inducing CD4(+) T cell and memory B cell response in the elderly (60 years or over) as in the adult population (18-59 years).

Published

2010

32. Seasonal influenza vaccine elicits heterosubtypic immunity against H5N1 that can be further boosted by H5N1 vaccination

Author

P. Noel Barrett, M. Keith Howard, Otfried Kistner, Michael G. Schwendinger, André van Maurik, Nicolas Sabarth, Helga Savidis Dacho, Peter Brühl, and Brian A. Crowe

Subjects

H5N1 vaccine, animal diseases, Orthomyxoviridae, Immunization, Secondary, Cross Reactions, medicine.disease_cause, Antibodies, Viral, Virus, Interferon-gamma, Mice, Orthomyxoviridae Infections, Immunity, Antibody Specificity, Neutralization Tests, medicine, Animals, Heterosubtypic immunity, Immunity, Cellular, General Veterinary, General Immunology and Microbiology, biology, Influenza A Virus, H5N1 Subtype, Public Health, Environmental and Occupational Health, Immunization, Passive, virus diseases, biology.organism_classification, Virology, Influenza A virus subtype H5N1, Immunity, Humoral, Vaccination, Infectious Diseases, Immunization, Influenza Vaccines, Immunology, Molecular Medicine, Female, Interleukin-4

Abstract

Recent findings indicate that seasonal influenza vaccination or infection of healthy humans may contribute to heterosubtypic immunity against new influenza A subtypes, such as H5N1. Here, we investigated whether seasonal influenza vaccination in a mouse model could induce any immunity against the H5N1 subtype. It could be demonstrated that, largely due to the H1N1 component strain A/NewCaledonia/20/99, parenteral immunization of mice with a trivalent seasonal influenza vaccine elicited heterosubtype H5-reactive antibodies able to confer partial protection against H5N1 influenza virus infection. Furthermore, the trivalent seasonal influenza vaccine was found to be compatible with a whole virus H5N1 vaccine in a heterologous prime-boost immunization regimen, achieving superior efficacy compared to a single immunization with an equivalent low-dose of the H5N1 vaccine.

Published

2009

33. Nonreplicating vaccinia virus vectors expressing the H5 influenza virus hemagglutinin produced in modified Vero cells induce robust protection

Author

Yee-Joo Tan, Brian A. Crowe, Annett Hessel, Helga Savidis-Dacho, Shen Shuo, Marijan Gerencer, Wanjing Hong, Otfried Kistner, Nicolas Sabarth, Michael G. Schwendinger, Peter Brühl, Georg Holzer, Sogue Coulibaly, Falko G. Falkner, P. Noel Barrett, Barbara Dietrich, and Josef Mayrhofer

Subjects

Virus Cultivation, Influenza vaccine, Immunology, Orthomyxoviridae, Genetic Vectors, Mice, Nude, Hemagglutinin Glycoproteins, Influenza Virus, Vaccinia virus, CD8-Positive T-Lymphocytes, medicine.disease_cause, Antibodies, Viral, Microbiology, Defective virus, chemistry.chemical_compound, Interferon-gamma, Mice, Orthomyxoviridae Infections, Virology, Chlorocebus aethiops, Vaccines and Antiviral Agents, medicine, Animals, Vero Cells, Duck embryo vaccine, Mice, Inbred BALB C, Attenuated vaccine, biology, Influenza A Virus, H5N1 Subtype, Defective Viruses, biology.organism_classification, Influenza A virus subtype H5N1, chemistry, Influenza Vaccines, Insect Science, Inactivated vaccine, Female, Vaccinia

Abstract

The timely development of safe and effective vaccines against avian influenza virus of the H5N1 subtype will be of the utmost importance in the event of a pandemic. Our aim was first to develop a safe live vaccine which induces both humoral and cell-mediated immune responses against human H5N1 influenza viruses and second, since the supply of embryonated eggs for traditional influenza vaccine production may be endangered in a pandemic, an egg-independent production procedure based on a permanent cell line. In the present article, the generation of a complementing Vero cell line suitable for the production of safe poxviral vaccines is described. This cell line was used to produce a replication-deficient vaccinia virus vector H5N1 live vaccine, dVV-HA5, expressing the hemagglutinin of a virulent clade 1 H5N1 strain. This experimental vaccine was compared with a formalin-inactivated whole-virus vaccine based on the same clade and with different replicating poxvirus-vectored vaccines. Mice were immunized to assess protective immunity after high-dose challenge with the highly virulent A/Vietnam/1203/2004(H5N1) strain. A single dose of the defective live vaccine induced complete protection from lethal homologous virus challenge and also full cross-protection against clade 0 and 2 challenge viruses. Neutralizing antibody levels were comparable to those induced by the inactivated vaccine. Unlike the whole-virus vaccine, the dVV-HA5 vaccine induced substantial amounts of gamma interferon-secreting CD8 T cells. Thus, the nonreplicating recombinant vaccinia virus vectors are promising vaccine candidates that induce a broad immune response and can be produced in an egg-independent and adjuvant-independent manner in a proven vector system.

Published

2009

34. Cell culture (Vero) derived whole virus (H5N1) vaccine based on wild-type virus strain induces cross-protective immune responses

Author

Martin Spruth, Ian Livey, Brian A. Crowe, Leopold Grillberger, Marijan Gerencer, P. Noel Barrett, Wolfgang Mundt, Falko G. Falkner, M. Keith Howard, Christa Tauer, Manfred Reiter, Walter Wodal, Helga Savidis-Dacho, Ines Mayerhofer, Peter Brühl, and Otfried Kistner

Subjects

H5N1 vaccine, Influenza vaccine, Guinea Pigs, Biology, Cross Reactions, medicine.disease_cause, Recombinant virus, Virus, Article, Microbiology, Mice, Orthomyxoviridae Infections, Chlorocebus aethiops, medicine, Influenza A virus, Animals, Vero Cells, Duck embryo vaccine, General Veterinary, General Immunology and Microbiology, Influenza A Virus, H5N1 Subtype, Public Health, Environmental and Occupational Health, T-Lymphocytes, Helper-Inducer, Virology, Influenza A virus subtype H5N1, Infectious Diseases, Vaccines, Inactivated, Influenza Vaccines, Vero cell, Molecular Medicine

Abstract

The rapid spread and the transmission to humans of avian influenza virus (H5N1) have induced world-wide fears of a new pandemic and raised concerns over the ability of standard influenza vaccine production methods to rapidly supply sufficient amounts of an effective vaccine. We report here on a robust and flexible strategy which uses wild-type virus grown in a continuous cell culture (Vero) system to produce an inactivated whole virus vaccine. Candidate vaccines based on clade 1 and clade 2 influenza H5N1 strains were developed and demonstrated to be highly immunogenic in animal models. The vaccines induce cross-neutralising antibodies, highly cross-reactive T-cell responses and are protective in a mouse challenge model not only against the homologous virus but also against other H5N1 strains, including those from another clade. These data indicate that cell culture-grown whole virus vaccines, based on the wild-type virus, allow the rapid high yield production of a candidate pandemic vaccine.

Published

2006

35. Improvement of the immune response against plasmid DNA encoding OspC of Borrelia by an ER-targeting leader sequence

Author

Peter Strasser, Ian Livey, Michael Breitenbach, Brian A. Crowe, Friedrich Dorner, Sven Mostböck, Richard Weiss, Arnulf Josef Hartl, Johann Dürnberger, Sandra Scheiblhofer, and Josef Thalhamer

Subjects

DNA, Bacterial, Cellular immunity, Molecular Sequence Data, Biology, Protein Sorting Signals, Endoplasmic Reticulum, law.invention, Interferon-gamma, Mice, Plasmid, Antigen, law, Animals, Humans, Amino Acid Sequence, Borrelia burgdorferi, Gene, Antigens, Bacterial, Immunity, Cellular, General Veterinary, General Immunology and Microbiology, Base Sequence, Immunogenicity, Borrelia, Public Health, Environmental and Occupational Health, Promoter, bacterial infections and mycoses, biology.organism_classification, Virology, Molecular biology, Antibodies, Bacterial, Infectious Diseases, Immunoglobulin G, Recombinant DNA, Molecular Medicine, Interleukin-4, Spleen, Bacterial Outer Membrane Proteins

Abstract

The present study outlines the characterization of a DNA-based immune response against the OspC antigen, one of the most promising candidates for a Borrelia vaccine. Balb/c mice were injected intradermally with plasmid DNA encoding the OspC gene (lacking the natural leader sequence) under transcriptional control of the cytomegalovirus (CMV) promotor. Immunization with this construct elicited only a marginal response, which was drastically improved by a fusion construct containing the human tissue plasminogen activator (hTPA) signal sequence. The results indicate that for DNA-based immunization against OspC an ER-targeting signal may be necessary for both antibody production as well as cellular immune responses.

Published

1999

36. Vectors Based on Modified Vaccinia Ankara Expressing Influenza H5N1 Hemagglutinin Induce Substantial Cross-Clade Protective Immunity

Author

Brian A. Crowe, Sogue Coulibaly, Annett Hessel, Marie-Luise Zips, Thomas R. Kreil, Hartmut J. Ehrlich, Klaus Orlinger, Georg Holzer, Falko G. Falkner, P. Noel Barrett, Michael G. Schwendinger, and Helga Savidis-Dacho

Subjects

Viral Diseases, Modified vaccinia Ankara, Anatomy and Physiology, Mouse, Cross Protection, viruses, lcsh:Medicine, medicine.disease_cause, Mice, Immune Physiology, Medicine, lcsh:Science, Clade, Immune Response, Vaccines, Multidisciplinary, biology, Vaccination, Animal Models, Infectious Diseases, Hemagglutinins, Research Article, Protective immunity, Clinical Research Design, Immunology, Genetic Vectors, Hemagglutinin (influenza), Vaccinia virus, Microbiology, Model Organisms, Species Specificity, Virology, Vaccine Development, Animals, Humans, Animal Models of Disease, Antigens, Biology, Influenza A Virus, H5N1 Subtype, Competing interests, business.industry, lcsh:R, Immunity, Viral Vaccines, Influenza, Influenza A virus subtype H5N1, Animal Models of Infection, Recombinant vaccines, biology.protein, Clinical Immunology, lcsh:Q, business

Abstract

BACKGROUND: New highly pathogenic H5N1 influenza viruses are continuing to evolve with a potential threat for an influenza pandemic. So far, the H5N1 influenza viruses have not widely circulated in humans and therefore constitute a high risk for the non immune population. The aim of this study was to evaluate the cross-protective potential of the hemagglutinins of five H5N1 strains of divergent clades using a live attenuated modified vaccinia Ankara (MVA) vector vaccine. METHODOLOGY/PRINCIPAL FINDINGS: The replication-deficient MVA virus was used to express influenza hemagglutinin (HA) proteins. Specifically, recombinant MVA viruses expressing the HA genes of the clade 1 virus A/Vietnam/1203/2004 (VN/1203), the clade 2.1.3 virus A/Indonesia/5/2005 (IN5/05), the clade 2.2 viruses A/turkey/Turkey/1/2005 (TT01/05) and A/chicken/Egypt/3/2006 (CE/06), and the clade 2.3.4 virus A/Anhui/1/2005 (AH1/05) were constructed. These experimental live vaccines were assessed in a lethal mouse model. Mice vaccinated with the VN/1203 hemagglutinin-expressing MVA induced excellent protection against all the above mentioned clades. Also mice vaccinated with the IN5/05 HA expressing MVA induced substantial protection against homologous and heterologous AH1/05 challenge. After vaccination with the CE/06 HA expressing MVA, mice were fully protected against clade 2.2 challenge and partially protected against challenge of other clades. Mice vaccinated with AH1/05 HA expressing MVA vectors were only partially protected against homologous and heterologous challenge. The live vaccines induced substantial amounts of neutralizing antibodies, mainly directed against the homologous challenge virus, and high levels of HA-specific IFN-γ secreting CD4 and CD8 T-cells against epitopes conserved among the H5 clades and subclades. CONCLUSIONS/SIGNIFICANCE: The highest level of cross-protection was induced by the HA derived from the VN/1203 strain, suggesting that pandemic H5 vaccines utilizing MVA vector technology, should be based on the VN/1203 hemagglutinin. Furthermore, the recombinant MVA-HA-VN, as characterized in the present study, would be a promising candidate for such a vaccine.

Published

2011

37. A Whole Virus Pandemic Influenza H1N1 Vaccine Is Highly Immunogenic and Protective in Active Immunization and Passive Protection Mouse Models

Author

Brian A. Crowe, Michael Graninger, Christa Tauer, Otfried Kistner, Wolfgang Mundt, Astrid Kerschbaum, P. Noel Barrett, Ines Mayerhofer, Nicolas Sabarth, Helga Savidis-Dacho, Alois Sachslehner, Peter Brühl, Leopold Grillberger, Hartmut J. Ehrlich, Falko G. Falkner, Manfred Reiter, Michael G. Schwendinger, Thomas R. Kreil, and Walter Wodal

Subjects

H5N1 vaccine, Swine, Science, viruses, Immunology, Mice, SCID, Biology, Active immunization, medicine.disease_cause, Virus, Disease Outbreaks, Mice, Influenza A Virus, H1N1 Subtype, Th2 Cells, Orthomyxoviridae Infections, Virology, Immunology/Immunity to Infections, Influenza, Human, Influenza A virus, medicine, Animals, Humans, Viremia, Virology/Vaccines, Duck embryo vaccine, Mice, Inbred BALB C, Multidisciplinary, Influenza A Virus, H5N1 Subtype, Viral Vaccine, Vaccination, virus diseases, Viral Vaccines, Th1 Cells, Virology/New Therapies, including Antivirals and Immunotherapy, Influenza A virus subtype H5N1, Disease Models, Animal, Treatment Outcome, Influenza Vaccines, Immunology/Immune Response, Medicine, Research Article

Abstract

The recent emergence and rapid spread of a novel swine-derived H1N1 influenza virus has resulted in the first influenza pandemic of this century. Monovalent vaccines have undergone preclinical and clinical development prior to initiation of mass immunization campaigns. We have carried out a series of immunogenicity and protection studies following active immunization of mice, which indicate that a whole virus, nonadjuvanted vaccine is immunogenic at low doses and protects against live virus challenge. The immunogenicity in this model was comparable to that of a whole virus H5N1 vaccine, which had previously been demonstrated to induce high levels of seroprotection in clinical studies. The efficacy of the H1N1 pandemic vaccine in protecting against live virus challenge was also seen to be equivalent to that of the H5N1 vaccine. The protective efficacy of the H1N1 vaccine was also confirmed using a severe combined immunodeficient (SCID) mouse model. It was demonstrated that mouse and guinea pig immune sera elicited following active H1N1 vaccination resulted in 100% protection of SCID mice following passive transfer of immune sera and lethal challenge. The immune responses to a whole virus pandemic H1N1 and a split seasonal H1N1 vaccine were also compared in this study. It was demonstrated that the whole virus vaccine induced a balanced Th-1 and Th-2 response in mice, whereas the split vaccine induced mainly a Th-2 response and only minimal levels of Th-1 responses. These data supported the initiation of clinical studies with the same low doses of whole virus vaccine that had previously been demonstrated to be immunogenic in clinical studies with a whole virus H5N1 vaccine.

Published

2010

38. A candidate OspC Lyme disease vaccine under clinical investigation

Author

Noel Barrett, I. Livey, Friedrich Dorner, Brian A. Crowe, Alexandra Löw-Baselli, Gerald Eder, and Marijan Gerencer

Subjects

Lyme disease, business.industry, Clinical investigation, Immunology, medicine, medicine.disease, business, LYME DISEASE VACCINE

Published

1999

39. Molecular properties of succinate dehydrogenase isolated from Micrococcus luteus (lysodeikticus)

Author

Brian A. Crowe and Peter Owen

Subjects

Immunodiffusion, Enzyme complex, Cytochrome, Macromolecular Substances, Octoxynol, Micrococcus, Flavin group, Cross Reactions, Microbiology, Cofactor, Polyethylene Glycols, Immunoelectrophoresis, Molecular Biology, biology, Succinate dehydrogenase, biology.organism_classification, Molecular biology, Molecular Weight, Succinate Dehydrogenase, Biochemistry, biology.protein, Electrophoresis, Polyacrylamide Gel, Micrococcus roseus, Micrococcus luteus, Research Article

Abstract

Succinate dehydrogenase (EC 1.3.99.1) of Micrococcus luteus was selectively precipitated from Triton X-100-solubilized membranes by using specific antiserum. The precipitated enzyme contained equimolar amounts of four polypeptides with apparent molecular weights of 72,000, 30,000, 17,000, and 15,000. The 72,000 polypeptide possessed a covalently bound flavin prosthetic group and appeared to be strongly antigenic as judged by immunoprinting experiments. Low-temperature absorption spectroscopy revealed the presence of cytochrome b556 in the antigen complex. By analogy with succinate dehydrogenase purified from other sources, the 72,000 and 30,000 polypeptides were considered to represent subunits of the succinate dehydrogenase enzyme, whereas one (or both) of the low-molecular-weight polypeptides was attributed to the apoprotein of the b-type cytochrome. A succinate dehydrogenase antigen cross-reacting with the M. luteus enzyme complex could be demonstrated in membranes of Micrococcus roseus, Micrococcus flavus, and Sarcina lutea, but not in the membranes isolated from a wide variety of other gram-positive and gram-negative bacteria.

Published

1983

40. Immunochemical analysis of respiratory-chain components of micrococcus luteus (lysodeikticus)

Author

Peter Owen and Brian A. Crowe

Subjects

Counterimmunoelectrophoresis, biology, Iron, NADPH Dehydrogenase, Respiratory chain, NADH Dehydrogenase, Dehydrogenase, Flavin group, Microbiology, Malate dehydrogenase, Levulinic Acids, Cofactor, Micrococcus, Succinate Dehydrogenase, Citric acid cycle, Oxygen Consumption, Biochemistry, Malate Dehydrogenase, Flavins, biology.protein, Oxidoreductases, Branched-chain alpha-keto acid dehydrogenase complex, Oxoglutarate dehydrogenase complex, Molecular Biology, Research Article

Abstract

Membrane-bound antigens of the respiratory chain of Micrococcus luteus were analyzed by crossed immunoelectrophoresis after growth of the organism in the presence of 59Fe, the flavin adenine dinucleotide-flavin mononucleotide precursor D-[2-14C]riboflavin, or the heme precursor 5-amino-[4-(14)C]levulinic acid. Using zymograms and procedures of selective extraction in conjunction with autoradiography, it was possible to resolve and partially characterize a number of antigens. Succinate dehydrogenase (EC 1.3.99.1) was shown to possess covalently bound flavin and nonheme iron and was possibly present as a complex with cytochrome. Three other dehydrogenases, namely, NADH dehydrogenase, NAD(P)H dehydrogenase (EC 1.6.99.3), and malate dehydrogenase (EC 1.1.1.37), contained flavin in noncovalent linkage, the NAD(P)H dehydrogenase also possessing nonheme iron. Four other discrete antigens (or antigen complexes) containing both iron and heme centers also resolved, as were two minor immunogens possessing iron as the sole detectable prosthetic group.

Published

1983

41. Characterization of succinate dehydrogenase from Micrococcus luteus (lysodeikticus) by electron-spin-resonance spectroscopy

Author

Peter Owen, Brian A. Crowe, Daulat S. Patil, and Richard Cammack

Subjects

Membrane potential, chemistry.chemical_classification, biology, Chemistry, Immunochemistry, Electron Spin Resonance Spectroscopy, Micrococcus, biology.organism_classification, Biochemistry, Redox, law.invention, Membrane Potentials, Succinate Dehydrogenase, Crystallography, Nuclear magnetic resonance, law, Oxidoreductase, Redox titration, Chemical Precipitation, Spectroscopy, Micrococcus luteus, Electron paramagnetic resonance, Oxidation-Reduction

Abstract

Low-temperature electron spin resonance spectroscopy has been used to study the biophysical properties of succinate dehydrogenase from the gram-positive bacterium Micrococcus luteus. The paramagnetic redox centres of the enzyme were identified in a succinate-dehydrogenase--antigen complex, which had been purified with the aid of monospecific serum from membranes solubilized with Triton X-100. The centres were characterized in further detail using the membrane-bound and Triton-solubilized forms of the enzyme. These studies distinguished two types of iron-sulphur centres, viz. a [4Fe-4S]3+ cluster displaying a narrow signal at g = 2.01 in the oxidized state (conventionally termed centre S-3) and a [2Fe-2S )0 cluster with an axial signal at g = 2.03 and 1.93 in the reduced state (conventionally termed centre S-1). Centre S-3 had a mid-point redox potential of +10 mV, a comparatively low value for this type of cluster. The behaviour of the g = 1.93 signal of centre S-1 was a complex function of the redox potential, microwave power and temperature of measurement. When measured at low power (i.e. non-saturating conditions), the intensities observed for the g = 1.93 signal poised at various critical potentials in the redox titration were similar. However, the corresponding intensities differed markedly at high power, where conditions were saturating. It is proposed that under saturating conditions the spin-lattice relaxation of the [2Fe-2S] cluster S-1 (mid-point potential +70 mV) is enhanced by centre S-3 between the potential range +10-+70 mV and by an ESR-silent centre, termed centre S-2, with a mid-point potential of -295 mV.

Published

1983

42. Study of the respiratory chain in Micrococcus luteus (lysodeikticus) by electron-spin-resonance spectroscopy

Author

Peter Owen, Brian A. Crowe, and Richard Cammack

Subjects

Stereochemistry, Iron, Respiratory chain, Heme, Biochemistry, Redox, law.invention, Membrane Potentials, Micrococcus, Electron Transport, Bacterial Proteins, law, medicine, Electron paramagnetic resonance, Oxidase test, biology, Chemistry, Succinate dehydrogenase, Cell Membrane, Electron Spin Resonance Spectroscopy, Membrane Proteins, biology.organism_classification, Membrane, Solubility, biology.protein, Ferric, Micrococcus luteus, Oxidation-Reduction, Copper, Sulfur, medicine.drug

Abstract

Low-temperature electron spin resonance spectroscopy was used to investigate the redox centres of Micrococcus luteus membranes. Three different types of iron-sulphur centres were distinguished. Two of these, a [4Fe-4S]3+-type cluster giving rise to a signal at g = 2.01 in the oxidized state and a [2Fe-2S] cluster with a spectrum at g = 2.03 and 1.93 in the reduced state, were attributable to succinate dehydrogenase. Another, generating signals in the reduced state at g = 2.027, 1.90 and 1.78 was identified as a 'Rieske' iron-sulphur centre. This latter cluster had a mid-point potential (pH 7.0) of +130 mV. In addition, signals characteristic of high-spin ferric haem (g = 6.20), low-spin ferric haem (g = 3.67, 3.36 and 3.01) and Cu2+ (g = 2.18 and 2.02) were also detected. The ferric-haem features, together with the Cu2+ and 'Rieske' centres, were enriched in membrane residues insoluble in Triton X-100, which are known from difference spectroscopy to contain cytochromes b-560, c-550 and a-601 (aa3 oxidase). The signals demonstrated by electron spin resonance for M. luteus membranes showed marked similarities to those documented for the complexes II, III, and IV of mitochondria. However, signals analogous to complex I (NADH-ubiquinone reductase) could not be demonstrated for M. luteus membranes.

Published

1983

43. Characterization of succinate dehydrogenase from Micrococcus lysodeikticus

Author

Peter Owen, Brian A. Crowe, and Richard Cammack

Subjects

biology, Biochemistry, Chemistry, Succinate dehydrogenase, biology.protein, Micrococcus lysodeikticus, Microbiology

Published

1982

44. British Entry into the Common Market: A British View

Author

Brian L. Crowe

Subjects

Power (social and political), Spanish Civil War, Commerce, Political science, Political economy, British Empire, World War II, Position (finance), Single market, Fall of man, Cost of living, Law

Abstract

The debate about Britain's entry into the Common Market has, at least in Britain herself, tended to focus on such relatively short-term matters as the cost of living and other immediate economic effects or the changes it would make in detailed aspects of the British way of life. This kind of debate is no doubt necessary and useful. After all, the short-term effects are not only the ones which have the most noticeable impact but ultimately become long-term ones. Nevertheless, this kind of debate ignores the very considerable changes which have been taking place steadily in the years-indeed decades-since the Second World War. British entry into the Common Market can be understood only in the longer-term perspective of British experience over this period and in the light of what we can expect in the future. We have to look at both the historical events and processes which brought us to our present situation and the prospects which are open to us. To see how we got where we are now, we must go back nearly three decades and look at our position in I945. Our future then was surely the least clearly charted of all the major participants in the Second World War, whether victors or vanquished. The United States and the Soviet Union were secure as superpowers. Germany, Japan, and Italy were all defeated and reconstruction had to be their single-minded aim. France had also been defeated; and while she, too, had overseas responsibilities, she had inevitably sacrificed less in an economic sense than we. We, having seen the war through from 194I to a victorious conclusion and having borne the burden of it alone from the fall of France until 194I, outwardly looked extremely powerful. With armies spread around the world we could be forgiven if we thought that the British Empire was at the height of its strength. But even in the years immediately after the war, the strains were beginning to show. The burden of fighting the Communists in Greece grew too heavy for us and we passed it to the United States. We found ourselves unable to solve the Palestine problem. We found that even as an apparently powerful victor-nation, unlike the United States and even the Soviet Union, our power had been undermined by the sacrifices of the war. We were, of course, a much smaller country than either of these; but, in addition, we continued to bear a combination of burdens which were too much for us.

Published

1972

45. Immunogenicity and protective efficacy of a Vero cell culture-derived whole-virus H7N9 vaccine in mice and guinea pigs.

Author

Walter Wodal, Michael G Schwendinger, Helga Savidis-Dacho, Brian A Crowe, Christine Hohenadl, Richard Fritz, Peter Brühl, Daniel Portsmouth, Anita Karner-Pichl, Dalida Balta, Leopold Grillberger, Otfried Kistner, P Noel Barrett, and M Keith Howard

Subjects

Medicine, Science

Abstract

BackgroundA novel avian H7N9 virus with a high case fatality rate in humans emerged in China in 2013. We evaluated the immunogenicity and protective efficacy of a candidate Vero cell culture-derived whole-virus H7N9 vaccine in small animal models.MethodsAntibody responses induced in immunized DBA/2J mice and guinea pigs were evaluated by hemagglutination inhibition (HI), microneutralization (MN), and neuraminidase inhibition (NAi) assays. T-helper cell responses and IgG subclass responses in mice were analyzed by ELISPOT and ELISA, respectively. Vaccine efficacy against lethal challenge with wild-type H7N9 virus was evaluated in immunized mice. H7N9-specific antibody responses induced in mice and guinea pigs were compared to those induced by a licensed whole-virus pandemic H1N1 (H1N1pdm09) vaccine.ResultsThe whole-virus H7N9 vaccine induced dose-dependent H7N9-specific HI, MN and NAi antibodies in mice and guinea pigs. Evaluation of T-helper cell responses and IgG subclasses indicated the induction of a balanced Th1/Th2 response. Immunized mice were protected against lethal H7N9 challenge in a dose-dependent manner. H7N9 and H1N1pdm09 vaccines were similarly immunogenic.ConclusionsThe induction of H7N9-specific antibody and T cell responses and protection against lethal challenge suggest that the Vero cell culture-derived whole-virus vaccine would provide an effective intervention against the H7N9 virus.

Published

2015