Your search keyword '"Lyons CR"' showing total 80 results

1. Intramuscular inoculation of Sin Nombre hantavirus cDNAs induces cellular and humoral immune responses in BALB/c mice

Author

Brian Hjelle, Lyons Cr, Mausumi Bharadwaj, and Ivo A. Wortman

Subjects

Orthohantavirus, Cellular immunity, DNA, Complementary, Hantavirus Infections, Blotting, Western, Biology, Antibodies, Viral, Lymphocyte Activation, Injections, Intramuscular, BALB/c, Mice, Neutralization Tests, Vaccines, DNA, Animals, Hantavirus, Immunity, Cellular, Mice, Inbred BALB C, General Veterinary, General Immunology and Microbiology, Sin Nombre virus, Immunogenicity, Public Health, Environmental and Occupational Health, Viral Vaccines, biology.organism_classification, Virology, Molecular biology, Infectious Diseases, DNA, Viral, Humoral immunity, biology.protein, Molecular Medicine, Antibody, Cell Division, Lymphoproliferative response

Abstract

To examine whether genetic immunization with Sin Nombre (SN) hantavirus genes could elicit immune responses, nine fragments spanning the envelope glycoprotein genes G1 and G2, and the complete N gene were cloned into a CMV expression vector. To ensure representation of all potential epitopes, adjacent fragments of the glycoprotein genes overlapped one another by 100 nucleotides. Vectors containing the gene fragments were inoculated intramuscularly into BALB/c mice and splenocyte proliferation and western blot-detectable antibodies and neutralization titers were determined. The N gene and seven of the nine M segment-derived cDNAs tested produced significant specific lymphoproliferative responses, and many of the constructs elicited either neutralizing or western blot-detectable antibodies. These promising results encourage the development of infection models for SN virus that will be capable of detecting protective responses.

Published

1999

2. Emerging roles of nitric oxide in inflammation

Author

Lyons Cr

Subjects

Inflammation, business.industry, Macrophages, General Medicine, Nitric Oxide, Leukocyte extravasation, Nitric oxide, chemistry.chemical_compound, chemistry, Immunology, medicine, Leukocytes, Animals, Humans, Endothelium, Vascular, medicine.symptom, business, Neuroscience, Homeostasis

Abstract

The short-lived, highly reactive NO radical arises in two ways: 1) a rapidly triggered process well suited for homeostatic fine-tuning of blood pressure and 2) a prolonged high-level production best suited for microbicidal activity. Roles in vascular "leakiness" and leukocyte extravasation are also emerging. Continued investigation may yield new therapies addressing individual facets of inflammation.

Published

1996

3. The Role of Nitric Oxide in Inflammation

Author

Lyons Cr

Subjects

Nitric Oxide Synthase Inhibitors, Endothelium, Inflammation, Biology, Stimulus (physiology), Effector cell, Leukocyte extravasation, Nitric oxide, chemistry.chemical_compound, Immune system, medicine.anatomical_structure, chemistry, Immunology, medicine, medicine.symptom

Abstract

Publisher Summary This chapter examines the multiple roles that nitric oxide (NO) may play during the inflammatory response. The majority of data implicating a role for NO in inflammation is based on experiments using nitric oxide synthase inhibitors. Inflammation results from increases in vascular flow, alterations in endothelium that can lead to plasma protein and leukocyte extravasation, and finally, the emigration of leukocytes from the circulation to the site of injury with resultant activation of effector cell mechanisms. There is evidence that NO can play a role during each stage of inflammation; the chapter discusses NO in the context of each of these stages. Conflicting data exist in the literature regarding the role of NO during inflammation. Some conflicts arise because of differences in the experimental systems studied such as in the animal species used or in the type of inflammatory stimulus. However, other differences may represent distinct physiologic and pathologic effects of NO during different phases of inflammation. NO plays a multifaceted role in all phases of the inflammatory immune response depending on the source and quantity of NO produced. It is important in the development of therapeutic modalities based on NO biochemistry and biology to take all roles of NO into consideration when designing potential treatments.

Published

1995

4. Bacillus anthracis Overcomes an Amino Acid Auxotrophy by Cleaving Host Serum Proteins.

Author

Terwilliger A, Swick MC, Pflughoeft KJ, Pomerantsev A, Lyons CR, Koehler TM, and Maresso A

Subjects

Amino Acid Sequence, Amino Acids chemistry, Bacillus anthracis genetics, Bacterial Proteins metabolism, Blood Proteins chemistry, Culture Media chemistry, Heme metabolism, Hemoglobins, Humans, Iron metabolism, Molecular Sequence Data, Amino Acids metabolism, Bacillus anthracis metabolism, Blood Proteins metabolism, Serum chemistry

Abstract

Unlabelled: Bacteria sustain an infection by acquiring nutrients from the host to support replication. The host sequesters these nutrients as a growth-restricting strategy, a concept termed "nutritional immunity." Historically, the study of nutritional immunity has centered on iron uptake because many bacteria target hemoglobin, an abundant circulating protein, as an iron source. Left unresolved are the mechanisms that bacteria use to attain other nutrients from host sources, including amino acids. We employed a novel medium designed to mimic the chemical composition of human serum, and we show here that Bacillus anthracis, the causative agent of anthrax disease, proteolyzes human hemoglobin to liberate essential amino acids which enhance its growth. This property can be traced to the actions of InhA1, a secreted metalloprotease, and extends to at least three other serum proteins, including serum albumin. The results suggest that we must also consider proteolysis of key host proteins to be a way for bacterial pathogens to attain essential nutrients, and we provide an experimental framework to determine the host and bacterial factors involved in this process., Importance: The mechanisms by which bacterial pathogens acquire nutrients during infection are poorly understood. Here we used a novel defined medium that approximates the chemical composition of human blood serum, blood serum mimic (BSM), to better model the nutritional environment that pathogens encounter during bacteremia. Removing essential amino acids from BSM revealed that two of the most abundant proteins in blood-hemoglobin and serum albumin-can satiate the amino acid requirement for Bacillus anthracis, the causative agent of anthrax. We further demonstrate that hemoglobin is proteolyzed by the secreted protease InhA1. These studies highlight that common blood proteins can be a nutrient source for bacteria. They also challenge the historical view that hemoglobin is solely an iron source for bacterial pathogens., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

5. Lethal factor, but not edema factor, is required to cause fatal anthrax in cynomolgus macaques after pulmonary spore challenge.

Author

Hutt JA, Lovchik JA, Drysdale M, Sherwood RL, Brasel T, Lipscomb MF, and Lyons CR

Subjects

Animals, Antibodies, Bacterial blood, Female, Macaca, Male, Spores, Bacterial pathogenicity, Virulence, Virulence Factors metabolism, Anthrax microbiology, Antigens, Bacterial metabolism, Bacillus anthracis pathogenicity, Bacterial Toxins metabolism, Lung microbiology, Respiratory Tract Infections microbiology

Abstract

Inhalational anthrax is caused by inhalation of Bacillus anthracis spores. The ability of B. anthracis to cause anthrax is attributed to the plasmid-encoded A/B-type toxins, edema toxin (edema factor and protective antigen) and lethal toxin (lethal factor and protective antigen), and a poly-d-glutamic acid capsule. To better understand the contribution of these toxins to the disease pathophysiology in vivo, we used B. anthracis Ames strain and isogenic toxin deletion mutants derived from the Ames strain to examine the role of lethal toxin and edema toxin after pulmonary spore challenge of cynomolgus macaques. Lethal toxin, but not edema toxin, was required to induce sustained bacteremia and death after pulmonary challenge with spores delivered via bronchoscopy. After intravenous challenge with bacilli to model the systemic phase of infection, lethal toxin contributed to bacterial proliferation and subsequent host death to a greater extent than edema toxin. Deletion of protective antigen resulted in greater loss of virulence after intravenous challenge with bacilli than deletion of lethal toxin or edema toxin alone. These findings are consistent with the ability of anti-protective antigen antibodies to prevent anthrax and suggest that lethal factor is the dominant toxin that contributes to the escape of significant numbers of bacilli from the thoracic cavity to cause anthrax after inhalation challenge with spores., (Copyright © 2014 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.)

Published

2014

6. Live attenuated Francisella novicida vaccine protects against Francisella tularensis pulmonary challenge in rats and non-human primates.

Author

Chu P, Cunningham AL, Yu JJ, Nguyen JQ, Barker JR, Lyons CR, Wilder J, Valderas M, Sherwood RL, Arulanandam BP, and Klose KE

Subjects

Animals, Macaca fascicularis, Mice, Models, Animal, Rats, Inbred F344, Tularemia mortality, Tularemia prevention & control, Vaccination, Vaccines, Attenuated immunology, Bacterial Vaccines immunology, Francisella tularensis, Immunodominant Epitopes immunology, Tularemia immunology

Abstract

Francisella tularensis causes the disease tularemia. Human pulmonary exposure to the most virulent form, F. tularensis subsp. tularensis (Ftt), leads to high morbidity and mortality, resulting in this bacterium being classified as a potential biothreat agent. However, a closely-related species, F. novicida, is avirulent in healthy humans. No tularemia vaccine is currently approved for human use. We demonstrate that a single dose vaccine of a live attenuated F. novicida strain (Fn iglD) protects against subsequent pulmonary challenge with Ftt using two different animal models, Fischer 344 rats and cynomolgus macaques (NHP). The Fn iglD vaccine showed protective efficacy in rats, as did a Ftt iglD vaccine, suggesting no disadvantage to utilizing the low human virulent Francisella species to induce protective immunity. Comparison of specific antibody profiles in vaccinated rat and NHP sera by proteome array identified a core set of immunodominant antigens in vaccinated animals. This is the first report of a defined live attenuated vaccine that demonstrates efficacy against pulmonary tularemia in a NHP, and indicates that the low human virulence F. novicida functions as an effective tularemia vaccine platform.

Published

2014

7. Serologic evidence of human Rickettsia infection found in three locations in Panamá.

Author

Bermúdez SE, Lyons CR, García GG, Zaldíva YL, Gabster A, and Arteaga GB

Subjects

Agricultural Workers' Diseases epidemiology, Animals, Animals, Zoo parasitology, Antigens, Bacterial immunology, Arachnid Vectors microbiology, Disease Reservoirs parasitology, Endemic Diseases, Environmental Exposure, Fluorescent Antibody Technique, Indirect, Forests, Humans, Immunoglobulin G blood, Immunoglobulin G immunology, Ixodidae microbiology, Occupational Exposure, Panama epidemiology, Pets parasitology, Rickettsia Infections immunology, Rickettsia rickettsii immunology, Rural Population, Seroepidemiologic Studies, Species Specificity, Surveys and Questionnaires, Tick Bites microbiology, Tick Infestations epidemiology, Tick Infestations prevention & control, Tick Infestations veterinary, Urban Population, Antibodies, Bacterial blood, Rickettsia immunology, Rickettsia Infections epidemiology

Abstract

Introduction: Since the middle of last century, cases of rickettsiosis have been found in Panamá when outbreaks of murine typhus and spotted fever were reported. Since then, little information exists about its prevalence in this country, since it is most often is misdiagnosed as another disease., Objectives: The aim of this paper is to demonstrate the presence of Rickettsia infections in humans in three locations in Panamá. These locations are agricultural areas, near forested areas or those who work in zoo., Materials and Methods: Three locations where chosen for this study: Tortí, El Valle de Antón and workers in the Summit Municipal Park in Panamá City. All volunteers signed an informed consent and answered a questionnaire. The samples were analyzed for the detection of rickettsial spotted fever and typhus group by the indirect immunofluorescence (using commercial kits) and antigens of Rickettsia rickettsii and R. amblyommii., Results: Blood samples were taken from 97 volunteers in Tortí (25), El Valle de Anton (37) and Summit Municipal Park (35). Of these, a total of 38 (39%) samples reacted to one of the two methods: eight (32%) in Tortí, 18 (48%) in El valle and 12 (34%) in Summit Municipal Park., Conclusion: The results show a high prevalence of antibodies to Rickettsia belonging to the spotted fever group in each of the three study areas, in addition to presenting evidence of the typhus group Rickettsia in El Valle de Anton. These areas could be considered endemic for rickettsiosis as there are conditions for maintaining them.

Published

2013

8. IgG subclass and heavy chain domains contribute to binding and protection by mAbs to the poly γ-D-glutamic acid capsular antigen of Bacillus anthracis.

Author

Hovenden M, Hubbard MA, Aucoin DP, Thorkildson P, Reed DE, Welch WH, Lyons CR, Lovchik JA, and Kozel TR

Subjects

Animals, Anthrax microbiology, Antibodies, Monoclonal immunology, Antibody Affinity, Antigen-Antibody Reactions, Bacterial Capsules immunology, Glutamic Acid immunology, Immunoglobulin Class Switching, Immunoglobulin G chemistry, Mice, Mice, Inbred BALB C, Protein Structure, Tertiary, Anthrax immunology, Bacillus anthracis immunology, Immunoglobulin Constant Regions immunology, Immunoglobulin G immunology, Immunoglobulin Heavy Chains immunology

Abstract

Bacterial capsules are common targets for antibody-mediated immunity. The capsule of Bacillus anthracis is unusual among capsules because it is composed of a polymer of poly-γ-d-glutamic acid (γdPGA). We previously generated murine IgG3 monoclonal antibodies (mAbs) to γdPGA that were protective in a murine model of pulmonary anthrax. IgG3 antibodies are characteristic of the murine response to polysaccharide antigens. The goal of the present study was to produce subclass switch variants of the γdPGA mAbs (IgG3 → IgG1 → IgG2b → IgG2a) and assess the contribution of subclass to antibody affinity and protection. Subclass switch antibodies had identical variable regions but differed in their heavy chains. The results showed that a switch from the protective IgG3 to IgG1, IgG2b or IgG2a was accompanied by i) a loss of protective activity ii) a change in mAb binding to the capsular matrix, and iii) a loss of affinity. These results identify a role for the heavy chain constant region in mAb binding. Hybrid mAbs were constructed in which the CH1, CH2 or CH3 heavy chain constant domains from a non-protective, low binding IgG2b mAb were swapped into the protective IgG3 mAb. The IgG3 mAb that contained the CH1 domain from IgG2b showed no loss of affinity or protection. In contrast, swapping the CH2 or CH3 domains from IgG2b into IgG3 produced a reduction in affinity and a loss of protection. These studies identify a role for the constant region of IgG heavy chains in affinity and protection against an encapsulated bacterial pathogen.

Published

2013

9. Autophagy protects against active tuberculosis by suppressing bacterial burden and inflammation.

Author

Castillo EF, Dekonenko A, Arko-Mensah J, Mandell MA, Dupont N, Jiang S, Delgado-Vargas M, Timmins GS, Bhattacharya D, Yang H, Hutt J, Lyons CR, Dobos KM, and Deretic V

Subjects

Animals, Autophagy genetics, Autophagy-Related Protein 5, Interleukin-17 immunology, Interleukin-1alpha genetics, Interleukin-1alpha immunology, Macrophages immunology, Mice, Mice, Transgenic, Microtubule-Associated Proteins genetics, Neutrophil Infiltration genetics, Neutrophil Infiltration immunology, Neutrophils immunology, Neutrophils microbiology, T-Lymphocytes immunology, T-Lymphocytes microbiology, Tuberculosis genetics, Tuberculosis microbiology, Autophagy immunology, Microtubule-Associated Proteins immunology, Mycobacterium tuberculosis immunology, Tuberculosis immunology

Abstract

Autophagy is a cell biological pathway affecting immune responses. In vitro, autophagy acts as a cell-autonomous defense against Mycobacterium tuberculosis, but its role in vivo is unknown. Here we show that autophagy plays a dual role against tuberculosis: antibacterial and anti-inflammatory. M. tuberculosis infection of Atg5(fl/fl) LysM-Cre(+) mice relative to autophagy-proficient littermates resulted in increased bacillary burden and excessive pulmonary inflammation characterized by neutrophil infiltration and IL-17 response with increased IL-1α levels. Macrophages from uninfected Atg5(fl/fl) LysM-Cre(+) mice displayed a cell-autonomous IL-1α hypersecretion phenotype, whereas T cells showed propensity toward IL-17 polarization during nonspecific activation or upon restimulation with mycobacterial antigens. Thus, autophagy acts in vivo by suppressing both M. tuberculosis growth and damaging inflammation.

Published

2012

10. Expression of either lethal toxin or edema toxin by Bacillus anthracis is sufficient for virulence in a rabbit model of inhalational anthrax.

Author

Lovchik JA, Drysdale M, Koehler TM, Hutt JA, and Lyons CR

Subjects

Animals, Anthrax mortality, Antigens, Bacterial genetics, Bacterial Capsules genetics, Bacterial Toxins genetics, Disease Models, Animal, Female, Gene Deletion, Histocytochemistry, Rabbits, Survival Analysis, Virulence, Anthrax microbiology, Anthrax pathology, Antigens, Bacterial biosynthesis, Bacillus anthracis pathogenicity, Bacterial Toxins biosynthesis, Virulence Factors biosynthesis

Abstract

The development of therapeutics against biothreats requires that we understand the pathogenesis of the disease in relevant animal models. The rabbit model of inhalational anthrax is an important tool in the assessment of potential therapeutics against Bacillus anthracis. We investigated the roles of B. anthracis capsule and toxins in the pathogenesis of inhalational anthrax in rabbits by comparing infection with the Ames strain versus isogenic mutants with deletions of the genes for the capsule operon (capBCADE), lethal factor (lef), edema factor (cya), or protective antigen (pagA). The absence of capsule or protective antigen (PA) resulted in complete avirulence, while the presence of either edema toxin or lethal toxin plus capsule resulted in lethality. The absence of toxin did not influence the ability of B. anthracis to traffic to draining lymph nodes, but systemic dissemination required the presence of at least one of the toxins. Histopathology studies demonstrated minimal differences among lethal wild-type and single toxin mutant strains. When rabbits were coinfected with the Ames strain and the PA- mutant strain, the toxin produced by the Ames strain was not able to promote dissemination of the PA- mutant, suggesting that toxigenic action occurs in close proximity to secreting bacteria. Taken together, these findings suggest that a major role for toxins in the pathogenesis of anthrax is to enable the organism to overcome innate host effector mechanisms locally and that much of the damage during the later stages of infection is due to the interactions of the host with the massive bacterial burden.

Published

2012

11. Identification of circulating bacterial antigens by in vivo microbial antigen discovery.

Author

Nuti DE, Crump RB, Dwi Handayani F, Chantratita N, Peacock SJ, Bowen R, Felgner PL, Davies DH, Wu T, Lyons CR, Brett PJ, Burtnick MN, Kozel TR, and AuCoin DP

Subjects

Animals, Burkholderia pseudomallei chemistry, Francisella tularensis chemistry, Immunoassay methods, Melioidosis microbiology, Mice, Mice, Inbred BALB C, Serum chemistry, Tularemia microbiology, Antigens, Bacterial blood, Bacteriological Techniques methods, Melioidosis diagnosis, Tularemia diagnosis

Abstract

Unlabelled: Detection of microbial antigens in clinical samples can lead to rapid diagnosis of an infection and administration of appropriate therapeutics. A major barrier in diagnostics development is determining which of the potentially hundreds or thousands of antigens produced by a microbe are actually present in patient samples in detectable amounts against a background of innumerable host proteins. In this report, we describe a strategy, termed in vivo microbial antigen discovery (InMAD), that we used to identify circulating bacterial antigens. This technique starts with "InMAD serum," which is filtered serum that has been harvested from BALB/c mice infected with a bacterial pathogen. The InMAD serum, which is free of whole bacterial cells, is used to immunize syngeneic BALB/c mice. The resulting "InMAD immune serum" contains antibodies specific for the soluble microbial antigens present in sera from the infected mice. The InMAD immune serum is then used to probe blots of bacterial lysates or bacterial proteome arrays. Bacterial antigens that are reactive with the InMAD immune serum are precisely the antigens to target in an antigen immunoassay. By employing InMAD, we identified multiple circulating antigens that are secreted or shed during infection using Burkholderia pseudomallei and Francisella tularensis as model organisms. Potential diagnostic targets identified by the InMAD approach included bacterial proteins, capsular polysaccharide, and lipopolysaccharide. The InMAD technique makes no assumptions other than immunogenicity and has the potential to be a broad discovery platform to identify diagnostic targets from microbial pathogens., Importance: Effective treatment of microbial infection is critically dependent on early diagnosis and identification of the etiological agent. One means for rapid diagnosis is immunoassay for antigens that are shed into body fluids during infection. Immunoassays can be inexpensive, rapid, and adaptable to a point-of-care format. A major impediment to immunoassay for diagnosis of infectious disease is identification of appropriate antigen targets. This report describes a strategy that can be used for identification of microbial antigens that are shed into serum during infection by the biothreats Burkholderia pseudomallei and Francisella tularensis. Termed InMAD (in vivo microbial antigen discovery), the strategy has the potential for application to a broad spectrum of microbial pathogens.

Published

2011

12. Cowpox virus inhibits human dendritic cell immune function by nonlethal, nonproductive infection.

Author

Hansen SJ, Rushton J, Dekonenko A, Chand HS, Olson GK, Hutt JA, Pickup D, Lyons CR, and Lipscomb MF

Subjects

Cell Survival, Cells, Cultured, Cytokines antagonists & inhibitors, Cytokines metabolism, Humans, NF-kappa B antagonists & inhibitors, NF-kappa B immunology, Cowpox virus immunology, Cowpox virus pathogenicity, Dendritic Cells immunology, Dendritic Cells virology, Immune Evasion

Abstract

Orthopoxviruses encode multiple proteins that modulate host immune responses. We determined whether cowpox virus (CPXV), a representative orthopoxvirus, modulated innate and acquired immune functions of human primary myeloid DCs and plasmacytoid DCs and monocyte-derived DCs (MDDCs). A CPXV infection of DCs at a multiplicity of infection of 10 was nonproductive, altered cellular morphology, and failed to reduce cell viability. A CPXV infection of DCs did not stimulate cytokine or chemokine secretion directly, but suppressed toll-like receptor (TLR) agonist-induced cytokine secretion and a DC-stimulated mixed leukocyte reaction (MLR). LPS-stimulated NF-κB nuclear translocation and host cytokine gene transcription were suppressed in CPXV-infected MDDCs. Early viral immunomodulatory genes were upregulated in MDDCs, consistent with early DC immunosuppression via synthesis of intracellular viral proteins. We conclude that a nonproductive CPXV infection suppressed DC immune function by synthesizing early intracellular viral proteins that suppressed DC signaling pathways., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

13. Antibodies contribute to effective vaccination against respiratory infection by type A Francisella tularensis strains.

Author

Mara-Koosham G, Hutt JA, Lyons CR, and Wu TH

Subjects

Animals, Antibodies, Bacterial blood, Antibodies, Bacterial therapeutic use, Cell Separation, Female, Flow Cytometry, Rats, Rats, Inbred F344, Rats, Nude, Respiratory Tract Infections prevention & control, Vaccination, Vaccines, Attenuated immunology, Antibodies, Bacterial immunology, Bacterial Vaccines immunology, Francisella tularensis immunology, Immunization, Passive, Respiratory Tract Infections immunology, Tularemia immunology, Tularemia prevention & control

Abstract

Pneumonic tularemia is a life-threatening disease caused by inhalation of the highly infectious intracellular bacterium Francisella tularensis. The most serious form of the disease associated with the type A strains can be prevented in experimental animals through vaccination with the attenuated live vaccine strain (LVS). The protection is largely cell mediated, but the contribution of antibodies remains controversial. We addressed this issue in a series of passive immunization studies in Fischer 344 (F344) rats. Subcutaneous LVS vaccination induced a robust serum antibody response dominated by IgM, IgG2a, and IgG2b antibodies. Prophylactic administration of LVS immune serum or purified immune IgG reduced the severity and duration of disease in naïve rats challenged intratracheally with a lethal dose of the virulent type A strain SCHU S4. The level of resistance increased with the volume of immune serum given, but the maximum survivable SCHU S4 challenge dose was at least 100-fold lower than that shown for LVS-vaccinated rats. Protection correlated with reduced systemic bacterial growth, less severe histopathology in the liver and spleen during the early phase of infection, and bacterial clearance by a T cell-dependent mechanism. Our results suggest that treatment with immune serum limited the sequelae associated with infection, thereby enabling a sterilizing T cell response to develop and resolve the infection. Thus, antibodies induced by LVS vaccination may contribute to the defense of F344 rats against respiratory infection by type A strains of F. tularensis.

Published

2011

14. Pre- and postexposure protection against virulent anthrax infection in mice by humanized monoclonal antibodies to Bacillus anthracis capsule.

Author

Chen Z, Schneerson R, Lovchik J, Lyons CR, Zhao H, Dai Z, Kubler-Kielb J, Leppla SH, and Purcell RH

Subjects

Amino Acid Sequence, Animals, Anthrax immunology, Anti-Infective Agents pharmacology, Humans, Immunoglobulin G chemistry, Kinetics, Mice, Mice, Inbred BALB C, Molecular Sequence Data, Pan troglodytes, Phagocytosis, Protein Binding, Sequence Homology, Amino Acid, Surface Plasmon Resonance, Anthrax prevention & control, Anthrax therapy, Antibodies, Monoclonal chemistry, Bacillus anthracis metabolism

Abstract

One of the two essential virulence factors of Bacillus anthracis is the poly-γ-D-glutamic acid (γDPGA) capsule. Five γDPGA-specific antibody antigen-binding fragments (Fabs) were generated from immunized chimpanzees. The two selected for further study, Fabs 11D and 4C, were both converted into full-length IgG1 and IgG3 mAbs having human IgG1 or IgG3 constant regions. These two mAbs had similar binding affinities, in vitro opsonophagocytic activities, and in vivo efficacies, with the IgG1 and IgG3 subclasses reacting similarly. The mAbs bound to γDPGA specifically with estimated binding affinities (K(d)) of 35-70 nM and effective affinities (effective K(d)) of 0.1-0.3 nM. The LD(50) in an opsonophagocytic bactericidal assay was ≈10 ng/mL of 11D or 4C. A single 30-μg dose of either mAb given to BALB/c mice 18 h before challenge conferred about 50% protection against a lethal intratracheal spore challenge by the virulent B. anthracis Ames strain. More importantly, either mAb given 8 h or 20 h after challenge provided significant protection against lethal infection. Thus, these anti-γDPGA mAbs should be useful, alone or in combination with antitoxin mAbs, for achieving a safe and efficacious postexposure therapy for anthrax.

Published

2011

15. Milestones in progression of primary pneumonic plague in cynomolgus macaques.

Author

Koster F, Perlin DS, Park S, Brasel T, Gigliotti A, Barr E, Myers L, Layton RC, Sherwood R, and Lyons CR

Subjects

Animals, Bacteremia microbiology, Body Temperature, Chemokines blood, Cytokines blood, Disease Progression, Electrocardiography, Female, Heart Rate, Lung microbiology, Lung pathology, Macaca fascicularis, Male, Monkey Diseases immunology, Monkey Diseases pathology, Monkey Diseases physiopathology, Plague immunology, Plague pathology, Plague physiopathology, Respiratory Rate, Reverse Transcriptase Polymerase Chain Reaction, Yersinia pestis immunology, Monkey Diseases microbiology, Plague microbiology

Abstract

Vaccines against primary pneumonic plague, a potential bioweapon, must be tested for efficacy in well-characterized nonhuman primate models. Telemetered cynomolgus macaques (Macaca fascicularis) were challenged by the aerosol route with doses equivalent to approximately 100 50% effective doses of Yersinia pestis strain CO92 and necropsied at 24-h intervals postexposure (p.e.). Data for telemetered heart rates, respiratory rates, and increases in the temperature greater than the diurnal baseline values identified the onset of the systemic response at 55 to 60 h p.e. in all animals observed for at least 70 h p.e. Bacteremia was detected at 72 h p.e. by a Yersinia 16S rRNA-specific quantitative reverse transcription-PCR and was detected later by the culture method at the time of moribund necropsy. By 72 h p.e. multilobar pneumonia with diffuse septal inflammation consistent with early bacteremia was established, and all lung tissues had a high bacterial burden. The levels of cytokines or chemokines in serum were not significantly elevated at any time, and only the interleukin-1beta, CCL2, and CCL3 levels were elevated in lung tissue. Inhalational plague in the cynomolgus macaque inoculated by the aerosol route produces most clinical features of the human disease, and in addition the disease progression mimics the disease progression from the anti-inflammatory phase to the proinflammatory phase described for the murine model. Defined milestones of disease progression, particularly the onset of fever, tachypnea, and bacteremia, should be useful for evaluating the efficacy of candidate vaccines.

Published

2010

16. The Fischer 344 rat reflects human susceptibility to francisella pulmonary challenge and provides a new platform for virulence and protection studies.

Author

Ray HJ, Chu P, Wu TH, Lyons CR, Murthy AK, Guentzel MN, Klose KE, and Arulanandam BP

Subjects

Animals, Bacterial Vaccines, Francisella tularensis growth & development, Humans, Macrophages microbiology, Models, Animal, Rats, Virulence, Disease Susceptibility diagnosis, Francisella tularensis pathogenicity, Lung microbiology, Rats, Inbred F344 microbiology, Tularemia therapy

Abstract

Background: The pathogenesis of Francisella tularensis, the causative agent of tularemia, has been primarily characterized in mice. However, the high degree of sensitivity of mice to bacterial challenge, especially with the human virulent strains of F. tularensis, limits this animal model for screening of defined attenuated vaccine candidates for protection studies., Methods and Findings: We analyzed the susceptibility of the Fischer 344 rat to pulmonary (intratracheal) challenge with three different subspecies (subsp) of F. tularensis that reflect different levels of virulence in humans, and characterized the bacterial replication profile in rat bone marrow-derived macrophages (BMDM). In contrast to the mouse, Fischer 344 rats exhibit a broader range of sensitivity to pulmonary challenge with the human virulent subsp. tularensis and holarctica. Unlike mice, Fischer rats exhibited a high degree of resistance to pulmonary challenge with LVS (an attenuated derivative of subsp. holarctica) and subsp. novicida. Within BMDM, subsp. tularensis and LVS showed minimal replication, subsp. novicida showed marginal replication, and subsp. holartica replicated robustly. The limited intramacrophage replication of subsp. tularensis and novicida strains was correlated with the induction of nitric oxide production. Importantly, Fischer 344 rats that survived pulmonary infection with subsp. novicida were markedly protected against subsequent pulmonary challenge with subsp. tularensis, suggesting that subsp. novicida may be a useful platform for the development of vaccines against subsp. tularensis., Conclusions: The Fischer 344 rat exhibits similar sensitivity to F. tularensis strains as that reported for humans, and thus the Fischer 344 ray may serve as a better animal model for tularemia vaccine development.

Published

2010

17. Regulatory interactions of a virulence-associated serine/threonine phosphatase-kinase pair in Bacillus anthracis.

Author

Shakir SM, Bryant KM, Larabee JL, Hamm EE, Lovchik J, Lyons CR, and Ballard JD

Subjects

Animals, Bacillus anthracis genetics, Bacterial Proteins genetics, Bacterial Proteins metabolism, Blotting, Western, Cell Line, Cells, Cultured, Electrophoresis, Polyacrylamide Gel, Mass Spectrometry, Mice, Mice, Inbred BALB C, Mutagenesis, Site-Directed, Myelin Basic Protein metabolism, Phosphopeptides metabolism, Phosphoprotein Phosphatases genetics, Phosphoprotein Phosphatases metabolism, Phosphorylation, Protein Binding, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Virulence genetics, Bacillus anthracis enzymology, Bacillus anthracis pathogenicity, Bacterial Proteins physiology, Phosphoprotein Phosphatases physiology, Protein Serine-Threonine Kinases physiology, Virulence physiology

Abstract

In the current study, we examined the regulatory interactions of a serine/threonine phosphatase (BA-Stp1), serine/threonine kinase (BA-Stk1) pair in Bacillus anthracis. B. anthracis STPK101, a null mutant lacking BA-Stp1 and BA-Stk1, was impaired in its ability to survive within macrophages, and this correlated with an observed reduction in virulence in a mouse model of pulmonary anthrax. Biochemical analyses confirmed that BA-Stp1 is a PP2C phosphatase and dephosphorylates phosphoserine and phosphothreonine residues. Treatment of BA-Stk1 with BA-Stp1 altered BA-Stk1 kinase activity, indicating that the enzymatic function of BA-Stk1 can be influenced by BA-Stp1 dephosphorylation. Using a combination of mass spectrometry and mutagenesis approaches, three phosphorylated residues, T165, S173, and S214, in BA-Stk1 were identified as putative regulatory targets of BA-Stp1. Further analysis found that T165 and S173 were necessary for optimal substrate phosphorylation, while S214 was necessary for complete ATP hydrolysis, autophosphorylation, and substrate phosphorylation. These findings provide insight into a previously undescribed Stp/Stk pair in B. anthracis.

Published

2010

18. The pathogenesis of acute pulmonary viral and bacterial infections: investigations in animal models.

Author

Lipscomb MF, Hutt J, Lovchik J, Wu T, and Lyons CR

Subjects

Adaptive Immunity, Animals, Immunity, Innate, Immunotherapy, Active, Macaca fascicularis, Mice, Rabbits, Rats, Respiratory Tract Infections immunology, Disease Models, Animal, Respiratory Tract Infections microbiology, Respiratory Tract Infections virology

Abstract

Acute viral and bacterial infections in the lower respiratory tract are major causes of morbidity and mortality worldwide. The proper study of pulmonary infections requires interdisciplinary collaboration among physicians and biomedical scientists to develop rational hypotheses based on clinical studies and to test these hypotheses in relevant animal models. Animal models for common lung infections are essential to understand pathogenic mechanisms and to clarify general mechanisms for host protection in pulmonary infections, as well as to develop vaccines and therapeutics. Animal models for uncommon pulmonary infections, such as those that can be caused by category A biothreat agents, are also very important because the infrequency of these infections in humans limits in-depth clinical studies. This review summarizes our understanding of innate and adaptive immune mechanisms in the lower respiratory tract and discusses how animal models for selected pulmonary pathogens can contribute to our understanding of the pathogenesis of lung infections and to the search for new vaccines and therapies.

Published

2010

19. New classes of orthopoxvirus vaccine candidates by functionally screening a synthetic library for protective antigens.

Author

Borovkov A, Magee DM, Loskutov A, Cano JA, Selinsky C, Zsemlye J, Lyons CR, and Sykes K

Subjects

Animals, Antibodies, Viral blood, Antibodies, Viral immunology, Antigens, Viral immunology, Cowpox virus immunology, Female, Gene Library, Mice, Mice, Inbred C57BL, Open Reading Frames, T-Lymphocytes immunology, Viral Vaccines immunology, Antigens, Viral genetics, Cowpox virus genetics, Genome, Viral, Viral Vaccines genetics

Abstract

The licensed smallpox vaccine, comprised of infectious vaccinia, is no longer popular as it is associated with a variety of adverse events. Safer vaccines have been explored such as further attenuated viruses and component designs. However, these alternatives typically provide compromised breadth and strength of protection. We conducted a genome-level screening of cowpox, the ancestral poxvirus, in the broadly immune-presenting C57BL/6 mouse as an approach to discovering novel components with protective capacities. Cowpox coding sequences were synthetically built and directly assayed by genetic immunization for open-reading frames that protect against lethal pulmonary infection. Membrane and non-membrane antigens were identified that partially protect C57BL/6 mice against cowpox and vaccinia challenges without adjuvant or regimen optimization, whereas the 4-pox vaccine did not. New vaccines might be developed from productive combinations of these new and existing antigens to confer potent, broadly efficacious protection and be contraindicated for none.

Published

2009

20. Vaccination of Fischer 344 rats against pulmonary infections by Francisella tularensis type A strains.

Author

Wu TH, Zsemlye JL, Statom GL, Hutt JA, Schrader RM, Scrymgeour AA, and Lyons CR

Subjects

Animals, Bacterial Vaccines administration & dosage, Disease Models, Animal, Female, Injections, Intradermal, Injections, Subcutaneous, Rats, Rats, Inbred F344, Survival Analysis, Bacterial Vaccines immunology, Francisella tularensis immunology, Tularemia pathology, Tularemia prevention & control

Abstract

Pneumonic tularemia caused by inhalation of the type A strains of Francisella tularensis is associated with high morbidity and mortality in humans. The only vaccine known to protect humans against this disease is the attenuated live vaccine strain (LVS), but it is not currently registered for human use. To develop a new generation of vaccines, multiple animal models are needed that reproduce the human response to F. tularensis infection and vaccination. We examined the potential use of Fischer 344 rat as such a model. Fischer 344 rats were very sensitive to intratracheal infection with the virulent type A strain SCHU S4 and generally succumbed less than 2 weeks after infection. Similar to humans and non-human primates, Fischer 344 rats vaccinated with LVS by subcutaneous or intradermal routes were protected against a greater range of respiratory SCHU S4 challenge doses than has been reported for LVS vaccinated mice. Intratracheal LVS vaccination also induced effective immunity, but it was less protective when the challenge dose exceeded 10(5) SCHU S4. LVS vaccination did not prevent SCHU S4 infection but rather controlled bacterial growth and pathology, leading to the eventual clearance of the bacteria. Our results suggest that the Fischer 344 rat may be a good model for studying pneumonic tularemia and evaluating potential vaccine candidates.

Published

2009

21. Rapid detection of the poly-gamma-D-glutamic acid capsular antigen of Bacillus anthracis by latex agglutination.

Author

AuCoin DP, Sutherland MD, Percival AL, Lyons CR, Lovchik JA, and Kozel TR

Subjects

Animals, Antigens, Bacterial immunology, Bacillus anthracis chemistry, Bacillus anthracis immunology, Bacterial Capsules immunology, Latex Fixation Tests methods, Mice, Mice, Inbred BALB C, Polyglutamic Acid analysis, Polyglutamic Acid immunology, Serum chemistry, Anthrax diagnosis, Antigens, Bacterial analysis, Bacillus anthracis isolation & purification, Bacterial Capsules chemistry, Polyglutamic Acid analogs & derivatives

Abstract

Latex agglutination has been used to detect capsular polysaccharides from a variety of bacteria in body fluids. A latex agglutination assay was constructed for detection of the poly-gamma-D-glutamic acid (gammaDPGA) capsular polypeptide of Bacillus anthracis in serum from animal models of pulmonary anthrax. The assay was able to detect gammaDPGA in serum from infected animals at concentrations of 100 to 200 ng/mL.

Published

2009

22. T cells from lungs and livers of Francisella tularensis-immune mice control the growth of intracellular bacteria.

Author

Collazo CM, Meierovics AI, De Pascalis R, Wu TH, Lyons CR, and Elkins KL

Subjects

Animals, Colony Count, Microbial, Female, Francisella tularensis growth & development, Interferon-gamma deficiency, Interferon-gamma immunology, Liver microbiology, Lung microbiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Spleen microbiology, Survival Analysis, Bacterial Vaccines immunology, Francisella tularensis immunology, Liver immunology, Lung immunology, T-Lymphocytes immunology, Tularemia prevention & control

Abstract

Parenteral and respiratory vaccinations with the intracellular bacterium Francisella tularensis have been studied using the live vaccine strain (LVS) in a mouse model, and spleen cells from immune mice are often used for immunological studies. However, mechanisms of host immunological responses may be different in nonlymphoid organs that are important sites of infection, such as lung and liver. Using parenteral (intradermal) or respiratory (cloud aerosol) vaccination, here we examine the functions of resulting LVS-immune liver or lung cells, respectively. Surprisingly, LVS was considerably more virulent when administered by cloud aerosol than by intranasal instillation, suggesting method-dependent differences in initial localization and/or dissemination patterns. Only low doses were sublethal, and resolution of sublethal cloud aerosol infection was dependent on gamma interferon (IFN-gamma), tumor necrosis factor alpha, and inducible nitric oxide synthase. Nonetheless, survival of cloud aerosol or parenteral infection resulted in the development of a protective immune response against lethal LVS intraperitoneal or aerosol challenge, reflecting development of systemic secondary immunity in both cases. Such immunity was further detected by directly examining the functions of LVS-immune lung or liver lymphocytes in vitro. Lung lymphocytes primed by respiratory infection, as well as liver lymphocytes primed by parenteral infection, clearly controlled in vitro intracellular bacterial growth primarily via mechanisms that were not dependent on IFN-gamma activity. Thus, our results indicate functional similarities between immune T cells residing in spleens, livers, and lungs of LVS-immune mice.

Published

2009

23. Killed but metabolically active Bacillus anthracis vaccines induce broad and protective immunity against anthrax.

Author

Skoble J, Beaber JW, Gao Y, Lovchik JA, Sower LE, Liu W, Luckett W, Peterson JW, Calendar R, Portnoy DA, Lyons CR, and Dubensky TW Jr

Subjects

Animals, Anthrax microbiology, Anthrax prevention & control, Anthrax Vaccines administration & dosage, Anthrax Vaccines genetics, Antigens, Bacterial immunology, Female, Furocoumarins, Guinea Pigs, Immunity, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Inbred DBA, Mutation, Rabbits, Spores, Bacterial genetics, Ultraviolet Rays, Vaccination, Vaccines, Inactivated administration & dosage, Vaccines, Inactivated genetics, Virulence, Anthrax immunology, Anthrax Vaccines immunology, Antibodies, Bacterial blood, Bacillus anthracis genetics, Bacillus anthracis immunology, Bacillus anthracis pathogenicity, Bacillus anthracis radiation effects, Vaccines, Inactivated immunology

Abstract

Bacillus anthracis is the causative agent of anthrax. We have developed a novel whole-bacterial-cell anthrax vaccine utilizing B. anthracis that is killed but metabolically active (KBMA). Vaccine strains that are asporogenic and nucleotide excision repair deficient were engineered by deleting the spoIIE and uvrAB genes, rendering B. anthracis extremely sensitive to photochemical inactivation with S-59 psoralen and UV light. We also introduced point mutations into the lef and cya genes, which allowed inactive but immunogenic toxins to be produced. Photochemically inactivated vaccine strains maintained a high degree of metabolic activity and secreted protective antigen (PA), lethal factor, and edema factor. KBMA B. anthracis vaccines were avirulent in mice and induced less injection site inflammation than recombinant PA adsorbed to aluminum hydroxide gel. KBMA B. anthracis-vaccinated animals produced antibodies against numerous anthrax antigens, including high levels of anti-PA and toxin-neutralizing antibodies. Vaccination with KBMA B. anthracis fully protected mice against challenge with lethal doses of toxinogenic unencapsulated Sterne 7702 spores and rabbits against challenge with lethal pneumonic doses of fully virulent Ames strain spores. Guinea pigs vaccinated with KBMA B. anthracis were partially protected against lethal Ames spore challenge, which was comparable to vaccination with the licensed vaccine anthrax vaccine adsorbed. These data demonstrate that KBMA anthrax vaccines are well tolerated and elicit potent protective immune responses. The use of KBMA vaccines may be broadly applicable to bacterial pathogens, especially those for which the correlates of protective immunity are unknown.

Published

2009

24. Characterization of BBB permeability in a preclinical model of cryptococcal meningoencephalitis using magnetic resonance imaging.

Author

Pai MP, Sakoglu U, Peterson SL, Lyons CR, and Sood R

Subjects

Animals, Blood-Brain Barrier pathology, Cerebral Cortex microbiology, Cerebral Cortex pathology, Cryptococcus neoformans growth & development, Injections, Intravenous, Male, Meningitis, Cryptococcal pathology, Meningitis, Cryptococcal physiopathology, Rats, Inbred F344, Time Factors, Blood-Brain Barrier microbiology, Capillary Permeability physiology, Disease Models, Animal, Magnetic Resonance Imaging methods, Meningitis, Cryptococcal microbiology, Rats

Abstract

Cryptococcus neoformans meningoencephalitis (CNME) is a leading fungal cause of death among acquired immunodeficiency syndrome patients. Innovative preclinical systems that permit high throughput in vivo evaluation of novel agents are desperately needed. Magnetic resonance imaging (MRI) was evaluated as a tool to develop a rat model of CNME and to quantify noninvasively blood-brain barrier (BBB) disruption secondary to this disease. The aim of this study was to identify MRI changes compared with histopathology and fungal burden measurements as potential biomarkers. A well-characterized strain of C neoformans (CN) var grubii was used to infect rats using intravenous inoculation. An inoculum-finding study was performed by infecting rats with 10(3), 10(5), and 10(7) colony-forming units (CFUs). Animals underwent dynamic MRI on days 4 and 7 after inoculation. An inoculum-confirming study was performed by infecting rats with 10(5), 10(6), and 10(7) CFU and fungal burden was determined in the brain, lung, and spleen. Animals infected with 10(7) CFU of CN developed lesions that appeared hyperintense on T2-weighted images on day 4. The histopathology results correlated well with MRI data. Diffusion weighted and permeability estimates were 1.4 and 6.1-fold higher, respectively, in lesions compared with healthy tissue. Magnetic resonance imaging is a promising preclinical tool to evaluate effects of antifungal and adjunctive agents.

Published

2009

25. Discriminating virulence mechanisms among Bacillus anthracis strains by using a murine subcutaneous infection model.

Author

Chand HS, Drysdale M, Lovchik J, Koehler TM, Lipscomb MF, and Lyons CR

Subjects

Animals, Antigens, Bacterial genetics, Antigens, Bacterial physiology, Bacterial Toxins genetics, Female, Lethal Dose 50, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Phagocytes immunology, Phagocytes microbiology, Survival Analysis, Virulence, Virulence Factors genetics, Anthrax microbiology, Anthrax pathology, Bacillus anthracis pathogenicity, Virulence Factors physiology

Abstract

Bacillus anthracis strains harboring virulence plasmid pXO1 that encodes the toxin protein protective antigen (PA), lethal factor, and edema factor and virulence plasmid pXO2 that encodes capsule biosynthetic enzymes exhibit different levels of virulence in certain animal models. In the murine model of pulmonary infection, B. anthracis virulence was capsule dependent but toxin independent. We examined the role of toxins in subcutaneous (s.c.) infections using two different genetically complete (pXO1(+) pXO2(+)) strains of B. anthracis, strains Ames and UT500. Similar to findings for the pulmonary model, toxin was not required for infection by the Ames strain, because the 50% lethal dose (LD(50)) of a PA-deficient (PA(-)) Ames mutant was identical to that of the parent Ames strain. However, PA was required for efficient s.c. infection by the UT500 strain, because the s.c. LD(50) of a UT500 PA(-) mutant was 10,000-fold higher than the LD(50) of the parent UT500 strain. This difference between the Ames strain and the UT500 strain could not be attributed to differences in spore coat properties or the rate of germination, because s.c. inoculation with the capsulated bacillus forms also required toxin synthesis by the UT500 strain to cause lethal infection. The toxin-dependent phenotype of the UT500 strain was host phagocyte dependent, because eliminating Gr-1(+) phagocytes restored virulence to the UT500 PA(-) mutant. These experiments demonstrate that the dominant virulence factors used to establish infection by B. anthracis depend on the route of inoculation and the bacterial strain.

Published

2009

26. Effect of Bacillus anthracis virulence factors on human dendritic cell activation.

Author

Hahn AC, Lyons CR, and Lipscomb MF

Subjects

Bacillus anthracis metabolism, Cytokines biosynthesis, Cytokines immunology, Dendritic Cells metabolism, Humans, Spores, Bacterial metabolism, Virulence Factors metabolism, Bacillus anthracis pathogenicity, Cytokines metabolism, Dendritic Cells immunology, Spores, Bacterial pathogenicity, Virulence Factors immunology

Abstract

Bacillus anthracis possesses three primary virulence factors: capsule, lethal toxin (LT), and edema toxin (ET). Dendritic cells (DCs) are critical to innate and acquired immunity and represent potential targets for these factors. We examined the ability of B. anthracis spores and bacilli to stimulate human monocyte-derived DC (MDDC), primary myeloid DC (mDC), and plasmacytoid DC (pDC) cytokine secretion. Exposure of MDDCs and mDCs to spores or vegetative bacilli of the genetically complete strain UT500 induced significantly increased cytokine secretion. Spores lacking genes required for capsule biosynthesis stimulated significantly higher cytokine secretion than UT500 spores from mDCs, but not MDDCs. In contrast, bacilli lacking capsule stimulated significantly higher cytokine secretion than UT500 bacilli in both MDDCs and mDCs. Spores or bacilli lacking both LT and ET stimulated significantly higher cytokine secretion than UT500 spores or bacilli, respectively, in both mDCs and MDDCs. pDCs exposed to spores or bacilli did not produce significant amounts of cytokines even when virulence factors were absent. In conclusion, B. anthracis employs toxins as well as capsule to inhibit human MDDC and mDC cytokine secretion, whereas human pDCs respond poorly even when capsule or both toxins are absent.

Published

2008

27. A dual-purpose protein ligand for effective therapy and sensitive diagnosis of anthrax.

Author

Vuyisich M, Gnanakaran S, Lovchik JA, Lyons CR, and Gupta G

Subjects

Animals, Antigens, Bacterial genetics, Cell Line, Humans, Ligands, Mice, Models, Molecular, Protein Structure, Quaternary, Sensitivity and Specificity, Anthrax diagnosis, Anthrax therapy, Antigens, Bacterial chemistry, Antigens, Bacterial metabolism

Abstract

This article reports the design of a bivalent protein ligand with dual use in therapy and diagnosis of anthrax caused by Bacillus anthracis. The ligand specifically binds to PA and thereby blocks the intracellular delivery of LF and EF toxins that, respectively, cause cell lysis and edema. The ligand is a chimeric scaffold with two PA-binding domains (called VWA) linked to an IgG-Fc frame. Molecular modeling and binding measurements reveal that the VWA-Fc dimer binds to PA with high affinity (K(D)=0.2 nM). An in vitro bio-luminescence assay shows that VWA-Fc (at nanomolar concentration) protects mouse macrophages from lysis by PA/LF. In vivo studies demonstrate that VWA-Fc at low doses (approximately 50 microg/animal) are able to rescue animals from lethal doses of PA/LF and B. anthracis spores. Finally, VWA-Fc is utilized as the capture molecule in the sensitive (down to 30 picomolar) detection of PA using surface plasmon resonance.

Published

2008

28. Application of in vivo induced antigen technology (IVIAT) to Bacillus anthracis.

Author

Rollins SM, Peppercorn A, Young JS, Drysdale M, Baresch A, Bikowski MV, Ashford DA, Quinn CP, Handfield M, Hillman JD, Lyons CR, Koehler TM, Calderwood SB, and Ryan ET

Subjects

Animals, Bacillus anthracis genetics, Gene Expression Profiling, Macaca mulatta, Mice, Mice, Inbred BALB C, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Antigens, Bacterial immunology, Bacillus anthracis immunology

Abstract

In vivo induced antigen technology (IVIAT) is an immuno-screening technique that identifies bacterial antigens expressed during infection and not during standard in vitro culturing conditions. We applied IVIAT to Bacillus anthracis and identified PagA, seven members of a N-acetylmuramoyl-L-alanine amidase autolysin family, three P60 family lipoproteins, two transporters, spore cortex lytic protein SleB, a penicillin binding protein, a putative prophage holin, respiratory nitrate reductase NarG, and three proteins of unknown function. Using quantitative real-time PCR comparing RNA isolated from in vitro cultured B. anthracis to RNA isolated from BALB/c mice infected with virulent Ames strain B. anthracis, we confirmed induced expression in vivo for a subset of B. anthracis genes identified by IVIAT, including L-alanine amidases BA3767, BA4073, and amiA (pXO2-42); the bacteriophage holin gene BA4074; and pagA (pXO1-110). The exogenous addition of two purified putative autolysins identified by IVIAT, N-acetylmuramoyl-L-alanine amidases BA0485 and BA2446, to vegetative B. anthracis cell suspensions induced a species-specific change in bacterial morphology and reduction in viable bacterial cells. Many of the proteins identified in our screen are predicted to affect peptidoglycan re-modeling, and our results support significant cell wall structural remodeling activity during B. anthracis infection. Identification of L-alanine amidases with B. anthracis specificity may suggest new potential therapeutic targets.

Published

2008

29. Clinical and pathologic features of cynomolgus macaques (Macaca fascicularis) infected with aerosolized Yersinia pestis.

Author

Van Andel R, Sherwood R, Gennings C, Lyons CR, Hutt J, Gigliotti A, and Barr E

Subjects

Aerosols, Animals, Anticonvulsants pharmacology, Anticonvulsants toxicity, Appetite drug effects, Bacterial Vaccines administration & dosage, Body Temperature drug effects, Chlorocebus aethiops microbiology, GABA Modulators pharmacology, GABA Modulators toxicity, Macaca mulatta microbiology, Motor Activity drug effects, Plague immunology, Species Specificity, Tiletamine pharmacology, Tiletamine toxicity, Zolazepam pharmacology, Zolazepam toxicity, Bacterial Vaccines therapeutic use, Macaca fascicularis microbiology, Plague microbiology, Plague veterinary, Plague Vaccine therapeutic use, Yersinia pestis pathogenicity

Abstract

Since the anthrax attacks of 2001, the emphasis on developing animal models of aerosolized select agent pathogens has increased. Many scientists believe that nonhuman primate models are the most appropriate to evaluate pulmonary response to, vaccines for, and treatments for select agents such as Yersinia pestis (Y. pestis), the causative agent of plague. A recent symposium concluded that the cynomolgus macaque (Macaca fascicularis) plague model should be characterized more fully. To date, a well-characterized cynomolgus macaque model of pneumonic plague using reproducible bioaerosols of viable Y. pestis has not been published. In the current study, methods for creating reproducible bioaerosols of viable Y. pestis strain CO92 (YpCO92) and pneumonic plague models were evaluated in 22 Indonesian-origin cynomolgus macaques. Five macaques exposed to doses lower than 250 CFU remained free of any indication of plague infection. Fifteen macaques developed fever, lethargy, and anorexia indicative of clinical plague. The 2 remaining macaques died without overt clinical signs but were plague-positive on culture and demonstrated pathology consistent with plague. The lethal dose of plague in humans is reputedly less than 100 organisms; in this study, 66 CFU was the dose at which half of the macaques developed fever and clinical signs (ED(50)), The Indonesian cynomolgus macaque reproduces many aspects of human pneumonic plague and likely will provide an excellent model for studies that require a macaque model.

Published

2008

30. Effects of endogenous D-alanine synthesis and autoinhibition of Bacillus anthracis germination on in vitro and in vivo infections.

Author

McKevitt MT, Bryant KM, Shakir SM, Larabee JL, Blanke SR, Lovchik J, Lyons CR, and Ballard JD

Subjects

Alanine antagonists & inhibitors, Alanine Racemase chemistry, Animals, Bacillus anthracis chemistry, Bacillus anthracis metabolism, Female, Macrophages immunology, Macrophages microbiology, Mice, Mice, Inbred BALB C, Mice, Inbred DBA, Spores, Bacterial chemistry, Spores, Bacterial growth & development, Spores, Bacterial metabolism, Stereoisomerism, Virulence, Alanine biosynthesis, Anthrax metabolism, Anthrax microbiology, Bacillus anthracis physiology

Abstract

Bacillus anthracis transitions from a dormant spore to a vegetative bacillus through a series of structural and biochemical changes collectively referred to as germination. The timing of germination is important during early steps in infection and may determine if B. anthracis survives or succumbs to responsive macrophages. In the current study experiments determined the contribution of endogenous D-alanine production to the efficiency and timing of B. anthracis spore germination under in vitro and in vivo conditions. Racemase-mediated production of endogenous D-alanine by B. anthracis altered the kinetics for initiation of germination over a range of spore densities and exhibited a threshold effect wherein small changes in spore number resulted in major changes in germination efficiency. This threshold effect correlated with D-alanine production, was prevented by an alanine racemase inhibitor, and required L-alanine. Interestingly, endogenous production of inhibitory levels of D-alanine was detected under experimental conditions that did not support germination and in a germination-deficient mutant of B. anthracis. Racemase-dependent production of D-alanine enhanced survival of B. anthracis during interaction with murine macrophages, suggesting a role for inhibition of germination during interaction with these cells. Finally, in vivo experiments revealed an approximately twofold decrease in the 50% lethal dose of B. anthracis spores administered in the presence of D-alanine, indicating that rates of germination may be directly influenced by the levels of this amino acid during early stages of disease.

Published

2007

31. Learning and modeling biosignatures from tissue images.

Author

Gilfeather F, Hamine V, Helman P, Hutt J, Loring T, Lyons CR, and Veroff R

Subjects

Algorithms, Animals, Bayes Theorem, Humans, Image Interpretation, Computer-Assisted, Infections classification, Lung anatomy & histology, Lung Diseases diagnosis, Mice, Artificial Intelligence, Computer Simulation, Diagnosis, Computer-Assisted, Infections diagnosis

Abstract

Ideally biosignatures can be detected at the early infection phase and used both for developing diagnostic patterns and for prognostic triage. Such biosignatures are important for vaccine validation and to provide risk stratification to a population such as for the identification of individuals who are exposed to biological or chemical agents and who are at high risk for developing an infection. The research goal is to detect broad based biosignature models and is initially focused on developing effective computer-augmented pathology tied to animal models developed at the University of New Mexico (UNM). Using lung tissue from infected and nai ve mice, feature extraction from images of the tissue under a specialized microscope, and Bayesian networks to analyze the data sets of features, we were able to differentiate normal from diseased samples and viral from bacterial samples in mid to late stages of infection. This effort has shown the potential effectiveness of computer-augmented pathology in this application. The extended research intends to couple analysis of serum, microarray analysis of organs, proteomic data and the pathology. The rational for the current invasive procedure on animal models is to facilitate the development of data analysis and machine learning techniques that can eventually be generalized to the task of discovering non-invasive and early stage biosignatures for human models.

Published

2007

32. Novel semisynthetic derivative of antibiotic Eremomycin active against drug-resistant gram-positive pathogens including Bacillus anthracis.

Author

Maples KR, Wheeler C, Ip E, Plattner JJ, Chu D, Zhang YK, Preobrazhenskaya MN, Printsevskaya SS, Solovieva SE, Olsufyeva EN, Heine H, Lovchik J, and Lyons CR

Subjects

Animals, Anthrax mortality, Anthrax prevention & control, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Glycopeptides chemistry, Glycopeptides pharmacology, Mice, Microbial Sensitivity Tests, Staphylococcal Infections mortality, Staphylococcal Infections prevention & control, Staphylococcus aureus drug effects, Structure-Activity Relationship, Anti-Bacterial Agents chemical synthesis, Bacillus anthracis drug effects, Drug Resistance, Bacterial, Glycopeptides chemical synthesis, Gram-Positive Bacteria drug effects

Abstract

Five adamantyl-containing carboxamides of eremomycin or vancomycin were synthesized and their antibacterial activities against some Gram-positive clinical isolates were investigated in vitro and in vivo. The adamantyl-2 amide of glycopeptide antibiotic eremomycin (1a in Chart 1, AN0900) was the most active compound and showed high activity against several Gram-positive pathogens: vancomycin-susceptible staphylococci and enterococci, glycopeptide-intermediate-resistant Staphylococcus aureus, and glycopeptide-resistant enterococci. Compound 1a was equally active in vitro against both Ciprofloxacin-susceptible and -resistant Bacillus anthracis strains (MICs 0.25-0.5 microg/mL). It was distinguished by having a 2.8 h half-life (t1/2) in mice and a volume of distribution of 2.18 L/kg. Compound 1a was active against Staphylococcus aureus in mice (iv) and provided complete protection against a lethal intravenous challenge with vegetative B. anthracis bacilli and also in a murine pulmonary anthrax model in which mice were challenged with Bacillus anthracis spores.

Published

2007

33. Murine innate immune response to virulent toxigenic and nontoxigenic Bacillus anthracis strains.

Author

Drysdale M, Olson G, Koehler TM, Lipscomb MF, and Lyons CR

Subjects

Animals, Anthrax microbiology, Anthrax pathology, Antigens, Bacterial genetics, Apoptosis, Bacillus anthracis pathogenicity, Bacterial Toxins genetics, Cell Survival, Colony Count, Microbial, Cytokines biosynthesis, Disease Models, Animal, Female, Immunity, Innate, In Situ Nick-End Labeling, Leukocyte Reduction Procedures, Mice, Mice, Inbred C57BL, Neutrophils immunology, Spleen immunology, Spleen microbiology, Spleen pathology, Anthrax immunology, Antigens, Bacterial biosynthesis, Bacillus anthracis immunology, Bacterial Toxins biosynthesis

Abstract

Effective treatment of anthrax is hampered by our limited understanding of the pathophysiology of Bacillus anthracis infection. We used a genetically complete (pXO1(+) pXO2(+)) virulent B. anthracis strain and four isogenic toxin-null mutants to determine the effects of the anthrax edema toxin (ET; edema factor [EF] plus protective antigen [PA]) and lethal toxin (LT; lethal factor [LF] plus PA) on the host innate response during systemic infection. Using the spleen as an indicator for host response, we found that intravenous inoculation of LT-deficient mutants into C57BL/6 mice significantly increased production of several cytokines over that observed after infection with the parent strain or an EF-deficient mutant. Bacteria producing one or both of the toxins were capable of inducing significant apoptosis of cells present in spleens, whereas apoptosis was greatly reduced in mice infected with nontoxigenic mutants. Mice infected with toxin-producing strains also showed increased splenic neutrophil recruitment compared to mice infected with nontoxigenic strains and neutrophil depletion prior to infection with toxin-producing strains, leading to decreased levels of apoptosis. Together, these studies indicate that anthrax LT suppresses cytokine secretion during infection, but both EF and LF play roles in inducing neutrophil recruitment and enhancing apoptosis. Interestingly, in the absence of LF the effect of EF-induced cell recruitment is further enhanced, perhaps because LF so effectively suppresses the secretion of chemokines.

Published

2007

34. Resolution of LPS-induced airway inflammation and goblet cell hyperplasia is independent of IL-18.

Author

Harris JF, Aden J, Lyons CR, and Tesfaigzi Y

Subjects

Animals, Bronchoalveolar Lavage Fluid immunology, Goblet Cells drug effects, Goblet Cells immunology, Hyperplasia, Inflammation etiology, Inflammation immunology, Inflammation pathology, Lung immunology, Male, Rats, Rats, Inbred F344, Respiratory Mucosa immunology, Goblet Cells pathology, Interleukin-18 physiology, Lipopolysaccharides toxicity, Lung pathology, Neutrophil Infiltration immunology, Respiratory Mucosa pathology

Abstract

Background: The resolution of inflammatory responses in the lung has not been described in detail and the role of specific cytokines influencing the resolution process is largely unknown., Methods: The present study was designed to describe the resolution of inflammation from 3 h through 90 d following an acute injury by a single intratracheal instillation of F344/N rats with LPS. We documented the inflammatory cell types and cytokines found in the bronchoalveolar lavage fluid (BALF), and epithelial changes in the axial airway and investigated whether IL-18 may play a role in the resolution process by reducing its levels with anti-IL-18 antibodies., Results: Three major stages of inflammation and resolution were observed in the BALF during the resolution. The first stage was characterized by PMNs that increased over 3 h to 1 d and decreased to background levels by d 6-8. The second stage of inflammation was characterized by macrophage influx reaching maximum numbers at d 6 and decreasing to background levels by d 40. A third stage of inflammation was observed for lymphocytes which were elevated over d 3-6. Interestingly, IL-18 and IL-9 levels in the BALF showed a cyclic pattern with peak levels at d 4, 8, and 16 while decreasing to background levels at d 1-2, 6, and 12. Depletion of IL-18 caused decreased PMN numbers at d 2, but no changes in inflammatory cell number or type at later time points., Conclusion: These data suggest that IL-18 plays a role in enhancing the LPS-induced neutrophilic inflammation of the lung, but does not affect the resolution of inflammation.

Published

2007

35. Protective and immunochemical activities of monoclonal antibodies reactive with the Bacillus anthracis polypeptide capsule.

Author

Kozel TR, Thorkildson P, Brandt S, Welch WH, Lovchik JA, AuCoin DP, Vilai J, and Lyons CR

Subjects

Animals, Anthrax prevention & control, Antibodies, Monoclonal therapeutic use, Antibody Affinity, Bacillus anthracis immunology, Bacterial Capsules chemistry, Disease Models, Animal, Lung Diseases immunology, Lung Diseases microbiology, Lung Diseases prevention & control, Mice, Mice, Inbred BALB C, Peptides immunology, Polymerase Chain Reaction, Anthrax immunology, Antibodies, Monoclonal immunology, Bacterial Capsules immunology, Glutamic Acid immunology

Abstract

Bacillus anthracis is surrounded by a polypeptide capsule composed of poly-gamma-d-glutamic acid (gammaDPGA). In a previous study, we reported that a monoclonal antibody (MAb F26G3) reactive with the capsular polypeptide is protective in a murine model of pulmonary anthrax. The present study examined a library of six MAbs generated from mice immunized with gammaDPGA. Evaluation of MAb binding to the capsule by a capsular "quellung" type reaction showed a striking diversity in capsular effects. Most MAbs produced a rim type reaction that was characterized by a sharp increase followed directly by a decrease in refractive index at the capsular edge. Some MAbs produced a second capsular reaction well beneath the capsular edge, suggesting complexity in capsular architecture. Binding of MAbs to soluble gammaDPGA was assessed by a fluorescence perturbation assay in which a change in the MAb intrinsic fluorescence produced by ligand binding was used as a reporter for antigen-antibody interaction. The MAbs differed considerably in the complexity of the binding curves. MAbs producing rim type capsule reactions typically produced the more complex binding isotherms. Finally, the protective activity of the MAbs was compared in a murine model of pulmonary anthrax. One MAb was markedly less protective than the remaining five MAbs. Characteristics of the more protective MAbs included a relatively high affinity, an immunoglobulin G3 isotype, and a complex binding isotherm in the fluorescence perturbation assay. Given the relatively monotonous structure of gammaDPGA, the results demonstrate a striking diversity in the antigen binding behavior of gammaDPGA antibodies.

Published

2007

36. Toxin-deficient mutants of Bacillus anthracis are lethal in a murine model for pulmonary anthrax.

Author

Heninger S, Drysdale M, Lovchik J, Hutt J, Lipscomb MF, Koehler TM, and Lyons CR

Subjects

Animals, Anthrax pathology, Antigens, Bacterial biosynthesis, Bacterial Capsules biosynthesis, Bacterial Capsules genetics, Bacterial Toxins biosynthesis, Disease Models, Animal, Female, Mice, Mice, Inbred BALB C, Pneumonia, Bacterial pathology, Spores, Bacterial genetics, Virulence Factors genetics, Anthrax microbiology, Anthrax mortality, Antigens, Bacterial genetics, Bacillus anthracis genetics, Bacillus anthracis pathogenicity, Bacterial Toxins genetics, Genes, Lethal, Pneumonia, Bacterial microbiology, Pneumonia, Bacterial mortality

Abstract

Bacillus anthracis, the etiologic agent of anthrax, produces at least three primary virulence factors: lethal toxin, edema toxin, and a capsule. The capsule is absolutely required for dissemination and lethality in a murine model of inhalation anthrax, yet the roles for the toxins during infection are ill-defined. We show in a murine model that when spores of specific toxin-null mutants are introduced into the lung, dissemination and lethality are comparable to those of the parent strain. Mutants lacking one or more of the structural genes for the toxin proteins, i.e., protective antigen, lethal factor, and edema factor, disseminated from the lung to the spleen at rates similar to that of the virulent parental strain. The 50% lethal dose (LD50) and mean time to death (MTD) of the mutants did not differ significantly from those of the parent. The LD50s or MTDs were also unaffected relative to those of the parent strain when mice were inoculated intravenously with vegetative cells. Nonetheless, histopathological examination of tissues revealed subtle but distinct differences in infections by the parent compared to some toxin mutants, suggesting that the host response is affected by toxin proteins synthesized during infection.

Published

2006

37. Expression profiling of Yersinia pestis during mouse pulmonary infection.

Author

Lawson JN, Lyons CR, and Johnston SA

Subjects

Administration, Intranasal, Animals, Base Composition, Bioterrorism, Cats, Colony Count, Microbial, Genomic Islands genetics, Liver microbiology, Mice, Mice, Inbred BALB C, Oligonucleotide Array Sequence Analysis, Plague Vaccine, RNA isolation & purification, Reverse Transcriptase Polymerase Chain Reaction, Spleen microbiology, Temperature, Transcription, Genetic, Yersinia pestis growth & development, Gene Expression Profiling methods, Lung microbiology, Plague genetics, Plague microbiology, Yersinia pestis genetics

Abstract

Yersinia pestis, the causative agent of plague, can be transmitted by infected flea bite or inhaled aerosol. Both routes of infection have a high mortality rate, and pneumonic infections of Y. pestis represent a significant concern as a tool of bioterrorism. Understanding the transcriptional program of this pathogen during pulmonary infection should be valuable in understanding plague pathogenesis, as well as potentially offering insights into new vaccines and therapeutics. Toward this goal we developed a long oligonucleotide microarray to the plague bacillus and evaluated the expression profiles of Y. pestis in vitro and in the mouse pulmonary infection model in vivo. The in vitro analysis compared expression patterns at 27 versus 37 degrees C, as a surrogate of the transition from the flea to the mammalian host. The in vivo analysis used intranasal challenge to the mouse lung. By amplifying the Y. pestis RNA from individual mouse lungs we were able to map the transcriptional profile of plague at postinfection days 1 to 3. Our data present a very different transcriptional profile between in vivo and in vitro expression, suggesting Y. pestis responds to a variety of host signals during infection. Of note was the number of genes found in genomic regions with altered %GC content that are upregulated within the mouse lung environment. These data suggest these regions may provide particularly promising targets for both vaccines and therapeutics.

Published

2006

38. Passive immunotherapy of Bacillus anthracis pulmonary infection in mice with antisera produced by DNA immunization.

Author

Herrmann JE, Wang S, Zhang C, Panchal RG, Bavari S, Lyons CR, Lovchik JA, Golding B, Shiloach J, and Lu S

Subjects

Animals, Anthrax immunology, Anthrax Vaccines immunology, Female, Mice, Mice, Inbred DBA, Pneumonia, Bacterial immunology, Rabbits, Vaccines, DNA immunology, Anthrax prevention & control, Anthrax Vaccines therapeutic use, Bacillus anthracis immunology, Immune Sera immunology, Immunization, Passive methods, Pneumonia, Bacterial prevention & control, Vaccines, DNA therapeutic use

Abstract

Because of the high failure rate of antibiotic treatment in patients with anthrax there is a need for additional therapies such as passive immunization with therapeutic antibodies. In this study, we used codon-optimized plasmid DNAs (DNA vaccines) encoding Bacillus anthracis protective antigen (PA) to immunize rabbits for producing anti-anthrax antibodies for use in passive immunotherapy. The antisera generated with these DNA vaccines were of high titer as measured by ELISA. The antisera were also able to protect J774 macrophage cells by neutralizing the cytotoxic effect of exogenously added anthrax lethal toxin, and of the toxin released by B. anthracis (Sterne strain) spores following infection. In addition, the antisera passively protected mice against pulmonary challenge with an approximate 50 LD50 dose of B. anthracis (Sterne strain) spores. The protection in mice was obtained when the antiserum was given 1h before or 1h after challenge. We further demonstrated that IgG and F(ab')2 components purified from anti-PA rabbit hyperimmune sera retained similar levels of neutralizing activities against both exogenously added B. anthracis lethal toxin and toxin produced by B. anthracis (Sterne strain) spores. The high titer antisera we produced will enable an immunization strategy to supplement antibiotic therapy for improving the survival of patients with anthrax.

Published

2006

39. Spontaneous reversion of Mycobacterium abscessus from a smooth to a rough morphotype is associated with reduced expression of glycopeptidolipid and reacquisition of an invasive phenotype.

Author

Howard ST, Rhoades E, Recht J, Pang X, Alsup A, Kolter R, Lyons CR, and Byrd TF

Subjects

Animals, Biofilms growth & development, Cells, Cultured, Culture Media, Disease Models, Animal, Humans, Lung microbiology, Mice, Mice, SCID, Monocytes cytology, Monocytes microbiology, Nontuberculous Mycobacteria genetics, Phenotype, Virulence, Glycolipids metabolism, Glycopeptides metabolism, Mycobacterium Infections, Nontuberculous microbiology, Nontuberculous Mycobacteria growth & development, Nontuberculous Mycobacteria pathogenicity

Abstract

Mycobacterium abscessus is an increasingly important cause of human disease; however, virulence determinants are largely uncharacterized. Previously, it was demonstrated that a rough, wild-type human clinical isolate (390R) causes persistent, invasive infection, while a smooth isogenic mutant (390S) has lost this capability. During serial passage of 390S, a spontaneous rough revertant was obtained, which was named 390V. This revertant regained the ability to cause persistent, invasive infection in human monocytes and the lungs of mice. Glycopeptidolipid (GPL), which plays a role in environmental colonization, was present in abundance in the cell wall of 390S, and was associated with sliding motility and biofilm formation. In contrast, a marked reduction in the amount of GPL in the cell wall of 390R and 390V was correlated with cord formation, a property associated with mycobacterial virulence. These results indicate that the ability to switch between smooth and rough morphologies may allow M. abscessus to transition between a colonizing phenotype and a more virulent, invasive form.

Published

2006

40. Gene transfer with inducible nitric oxide synthase decreases production of urea by arginase in pulmonary arterial endothelial cells.

Author

Stanley KP, Chicoine LG, Young TL, Reber KM, Lyons CR, Liu Y, and Nelin LD

Subjects

Adenoviridae genetics, Animals, Arginase antagonists & inhibitors, Arginine pharmacology, Cattle, Cell Proliferation drug effects, Cells, Cultured, Gene Expression Profiling, Genetic Vectors, NG-Nitroarginine Methyl Ester pharmacology, Nitric Oxide metabolism, Nitric Oxide Synthase Type II biosynthesis, Nitric Oxide Synthase Type III biosynthesis, Arginase metabolism, Endothelium, Vascular metabolism, Gene Transfer Techniques, Nitric Oxide Synthase Type II genetics, Pulmonary Artery cytology, Urea metabolism

Abstract

Nitric oxide (NO) is a vasodilator produced from L-arginine (L-Arg) by NO synthase (NOS). Gene therapy for hypertensive disorders has been proposed using the inducible isoform of NOS (iNOS). L-Arg also can be metabolized to urea and L-ornithine (L-Orn) by arginase, and L-Orn can be metabolized to proline and/or polyamines, which are vital for cellular proliferation. To determine the effect of iNOS gene transfer on arginase, we transfected bovine pulmonary arterial endothelial cells (bPAEC) with an adenoviral vector containing the gene for iNOS (AdiNOS). As expected, NO production in AdiNOS bPAEC was substantially greater than in control bPAEC. Although urea production was significantly less in the AdiNOS bPAEC than in the control bPAEC, despite similar levels of arginase I protein, AdiNOS transfection of bPAEC had no effect on the uptake of L-Arg. Inhibiting NO production with Nomega-nitro-L-arginine methyl ester increased urea production, and inhibiting urea production with L-valine increased nitrite production, in AdiNOS bPAEC. The addition of L-Arg to the medium increased urea production by AdiNOS bPAEC in a concentration-dependent manner. Thus, in these iNOS-transfected bPAEC, the transfected iNOS and native arginase compete for a common intracellular pool of L-Arg. This competition for substrate resulted in impaired proliferation in the AdiNOS-transfected bPAEC. These findings suggest that the use of iNOS gene therapy for pulmonary hypertensive disorders may not only be beneficial through NO-mediated pulmonary vasodilation but also may decrease vascular remodeling by limiting L-Orn production by native arginase.

Published

2006

41. Intranasal vaccination induces protective immunity against intranasal infection with virulent Francisella tularensis biovar A.

Author

Wu TH, Hutt JA, Garrison KA, Berliba LS, Zhou Y, and Lyons CR

Subjects

Administration, Intranasal, Animals, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Disease Models, Animal, Francisella tularensis immunology, Francisella tularensis pathogenicity, Humans, Injections, Subcutaneous, Mice, Mice, Inbred BALB C, Mice, Inbred C3H, Mice, Inbred C57BL, Mice, Inbred DBA, Tularemia immunology, Tularemia microbiology, Tularemia mortality, Vaccination, Virulence, Bacterial Vaccines administration & dosage, Bacterial Vaccines immunology, Tularemia prevention & control

Abstract

The inhalation of Francisella tularensis biovar A causes pneumonic tularemia associated with high morbidity and mortality rates in humans. Exposure to F. tularensis usually occurs by accident, but there is increasing awareness that F. tularensis may be deliberately released in an act of bioterrorism or war. The development of a vaccine against pneumonic tularemia has been limited by a lack of information regarding the mechanisms required to protect against this disease. Vaccine models for F. tularensis in inbred mice would facilitate investigations of the protective mechanisms and significantly enhance vaccine development. Intranasal vaccination with the attenuated live vaccine strain (LVS) of F. tularensis reproducibly protected BALB/c mice, but not C57BL/6 mice, against intranasal and subcutaneous challenges with a virulent clinical isolate of F. tularensis biovar A (NMFTA1). The resistance of LVS-vaccinated BALB/c mice to intranasal NMFTA1 challenge was increased 100-fold by boosting with live NMFTA1 but not with LVS. The protective response was specific for F. tularensis and required both CD4 and CD8 T cells. The vaccinated mice appeared outwardly healthy for more than 2 months after NMFTA1 challenge, even though NMFTA1 was recovered from more than half of the vaccinated mice. These results show that intranasal vaccination induces immunity that protects BALB/c mice from intranasal infection by F. tularensis biovar A.

Published

2005

42. Capsule synthesis by Bacillus anthracis is required for dissemination in murine inhalation anthrax.

Author

Drysdale M, Heninger S, Hutt J, Chen Y, Lyons CR, and Koehler TM

Subjects

Animals, Bacillus anthracis genetics, Disease Models, Animal, Female, Gene Expression Regulation, Bacterial, Lung microbiology, Lung pathology, Mice, Mice, Inbred BALB C, Operon, Spleen microbiology, Spleen pathology, Survival Rate, Virulence Factors genetics, Virulence Factors metabolism, Anthrax microbiology, Bacillus anthracis metabolism, Bacillus anthracis pathogenicity, Bacterial Capsules biosynthesis, Bacterial Capsules genetics

Abstract

Bacillus anthracis, the agent of anthrax, produces a poly-D-glutamic acid capsule that has been implicated in virulence. Many strains missing pXO2 (96 kb), which harbors the capsule biosynthetic operon capBCAD, but carrying pXO1 (182 kb) that harbors the anthrax toxin genes, are attenuated in animal models. Also, noncapsulated strains are readily phagocytosed by macrophage cell lines, whereas capsulated strains are resistant to phagocytosis. We show that a strain carrying both virulence plasmids but deleted specifically for capBCAD is highly attenuated in a mouse model for inhalation anthrax. The parent strain and capsule mutant initiated germination in the lungs, but the capsule mutant did not disseminate to the spleen. A mutant harboring capBCAD but deleted for the cap regulators acpA and acpB was also significantly attenuated, in agreement with the capsule-negative phenotype during in vitro growth. Surprisingly, an acpB mutant, but not an acpA mutant, displayed an elevated LD(50) and reduced ability to disseminate, indicating that acpA and acpB are not true functional homologs and that acpB may play a larger role in virulence than originally suspected.

Published

2005

43. Intratracheal adenoviral-mediated delivery of iNOS decreases pulmonary vasoconstrictor responses in rats.

Author

Chicoine LG, Tzeng E, Bryan R, Saenz S, Paffett ML, Jones J, Lyons CR, Resta TC, Nelin LD, and Walker BR

Subjects

15-Hydroxy-11 alpha,9 alpha-(epoxymethano)prosta-5,13-dienoic Acid pharmacology, Adenoviridae, Animals, Dose-Response Relationship, Drug, Exhalation, Genetic Vectors, Humans, Immunologic Techniques, In Vitro Techniques, Lung metabolism, Male, Nitric Oxide, Nitric Oxide Synthase genetics, Nitric Oxide Synthase metabolism, Nitric Oxide Synthase pharmacology, Nitric Oxide Synthase Type II, Rats, Rats, Sprague-Dawley, Staining and Labeling, Time Factors, Tissue Distribution, Trachea, Vascular Resistance drug effects, Vasoconstrictor Agents pharmacology, Nitric Oxide Synthase administration & dosage, Pulmonary Circulation drug effects, Transduction, Genetic methods, Vasoconstriction drug effects

Abstract

We hypothesized that adenovirus-mediated inducible nitric oxide synthase (iNOS) gene transduction of the lung would result in time-dependent iNOS overexpression and attenuate the vascular constrictor responses to a thromboxane mimetic, U-46619. Rats were treated via the trachea with surfactant alone (sham), surfactant containing an adenoviral construct with a cytomegalovirus promoter-regulated human iNOS gene (Adeno-iNOS), or an adenoviral construct without a gene insert (Adeno-Control). Adeno-iNOS-transduced rats demonstrated human iNOS mRNA and increased iNOS protein levels only in the lungs. Immunohistochemistry of lungs from Adeno-iNOS-treated animals demonstrated transgene expression in alveolar wall cells. In the lungs from Adeno-iNOS-transduced rats, the expression of iNOS protein and exhaled nitric oxide concentrations were increased on days 1-4 and 7 but returned to baseline values by day 14. The administration of the selective iNOS inhibitor L-N6-(1-iminoethyl)lysine dihydrochloride (L-NIL) decreased exhaled nitric oxide concentrations to levels found in Adeno-Control-transduced lungs. In a second group of rats, the segmental vasoconstrictor responses to U-46619 were determined in isolated, perfused lungs 3 days after transduction. Lungs from rats transduced with Adeno-iNOS had reduced total, arterial, and venous vasoconstrictor responses to U-46619 compared with sham, Adeno-Control, and control groups. In a third set of experiments, the response to 400 nM U-46619 in the presence of 10 microM L-NIL was not different in the isolated lungs from Adeno-Control- and Adeno-iNOS-transduced rats. We conclude that adenovirus-mediated iNOS gene transduction of the lung results in time-dependent iNOS overexpression, which attenuates the vascular constrictor responses to the thromboxane mimetic U-46619.

Published

2004

44. Organism identification using a genome sequence-independent universal microarray probe set.

Author

Belosludtsev YY, Bowerman D, Weil R, Marthandan N, Balog R, Luebke K, Lawson J, Johnston SA, Lyons CR, Obrien K, Garner HR, and Powdrill TF

Subjects

Bacillus anthracis genetics, Bacillus subtilis genetics, Bioterrorism, Gene Expression Profiling instrumentation, Molecular Sequence Data, Nucleic Acid Hybridization methods, Oligonucleotide Array Sequence Analysis methods, Streptococcus pneumoniae genetics, Yersinia pestis genetics, DNA Probes, DNA, Bacterial genetics, Gene Expression Profiling methods, Oligonucleotide Array Sequence Analysis instrumentation, Oligonucleotide Probes

Abstract

There has been increasing interest and efforts devoted to developing biosensor technologies for identifying pathogens, particularly in the biothreat area. In this study, a universal set of short 12- and 13-mer oligonucleotide probes was derived independently of a priori genomic sequence information and used to generate unique species-dependent genomic hybridization signatures. The probe set sequences were algorithmically generated to be maximally distant in sequence space and not dependent on the sequence of any particular genome. The probe set is universally applicable because it is unbiased and independent of hybridization predictions based upon simplified assumptions regarding probe-target duplex formation from linear sequence analysis. Tests were conducted on microarrays containing 14,283 unique probes synthesized using an in situ light-directed synthesis methodology. The genomic DNA hybridization intensity patterns reproducibly differentiated various organisms (Bacillus subtilis, Yersinia pestis, Streptococcus pneumonia, Bacillus anthracis, and Homo sapiens), including the correct identification of a blinded "unknown" sample. Applications of this method include not only pathological and forensic genome identification in medicine and basic science, but also potentially a novel method for the discovery of unknown targets and associations inherent in dynamic nucleic acid populations such as represented by differential gene expression.

Published

2004

45. Murine model of pulmonary anthrax: kinetics of dissemination, histopathology, and mouse strain susceptibility.

Author

Lyons CR, Lovchik J, Hutt J, Lipscomb MF, Wang E, Heninger S, Berliba L, and Garrison K

Subjects

Administration, Intranasal, Animals, Animals, Inbred Strains, Bacillus anthracis isolation & purification, Bacillus anthracis physiology, Disease Susceptibility, Female, Lung pathology, Male, Mice, Mice, Inbred BALB C, Species Specificity, Spleen pathology, Spores, Bacterial pathogenicity, Anthrax microbiology, Anthrax pathology, Anthrax physiopathology, Bacillus anthracis pathogenicity, Disease Models, Animal, Pneumonia, Bacterial microbiology, Pneumonia, Bacterial pathology, Pneumonia, Bacterial physiopathology

Abstract

Bioweapons are most often designed for delivery to the lung, although this route is not the usual portal of entry for many of the pathogens in the natural environment. Vaccines and therapeutics that are efficacious for natural routes of infection may not be effective against the pulmonary route. Pulmonary models are needed to investigate the importance of specific bacterial genes in virulence, to identify components of the host immune system that are important in providing innate and acquired protection, and for testing diagnostic and therapeutic strategies. This report describes the characteristics of host and Bacillus anthracis interactions in a murine pulmonary-infection model. The infective dose varied depending on the route and method of inoculation. The germination process in the lung began within 1 h of inoculation into the lung, although growth within the lung was limited. B. anthracis was found in the lung-associated lymph nodes approximately 5 h after infection. Minimal pneumonitis was associated with the lung infection, but significant systemic pathology was noted after dissemination. Infected mice typically succumbed to infection approximately 3 to 4 days after inoculation. The 50% lethal doses differed among inbred strains of mice, but within a given mouse strain, neither the age nor the sex of the mice influenced susceptibility to B. anthracis.

Published

2004

46. mAbs to Bacillus anthracis capsular antigen for immunoprotection in anthrax and detection of antigenemia.

Author

Kozel TR, Murphy WJ, Brandt S, Blazar BR, Lovchik JA, Thorkildson P, Percival A, and Lyons CR

Subjects

Animals, Anthrax immunology, Anthrax prevention & control, Antigens, Bacterial immunology, Enzyme-Linked Immunosorbent Assay, Mice, Anthrax diagnosis, Antibodies, Monoclonal immunology, Antigens, Bacterial blood, Bacillus anthracis immunology

Abstract

Bacillus anthracis is surrounded by an antiphagocytic polypeptide capsule composed of poly gamma-D-glutamic acid (gammaDPGA). gammaDPGA has been identified recently as a potential target for vaccine development. Studies of the role of gammaDPGA in disease have been hampered by the poor Ab response to this antigen and the lack of immunochemical reagents. As a consequence, neither the extent of gammaDPGA production during anthrax nor the protective activity of gammaDPGA Abs in inhalation anthrax are known. Here we report production of IgG Abs to gammaDPGA in mice following an immunization regimen using gammaDPGA in combination with agonist mAbs to CD40. mAbs were produced that are specific for gammaDPGA. Passive immunization with gammaDPGA mAbs protected >90% of mice in a pulmonary model of anthrax that was lethal in control mice (P < 0.0001). Use of gammaDPGA mAb in an antigen detection immunoassay found that the appearance of gammaDPGA in serum coincided with the emergence of bacteremia. These studies identify CD40 stimulation as a means for production of Ab and generation of mAbs against a weakly immunogenic antigen and demonstrate that the capsule is an effective target for immunoprotection and for antigen detection in the diagnosis of anthrax.

Published

2004

47. A polymorphic region in Mycobacterium abscessus contains a novel insertion sequence element.

Author

Howard ST, Byrd TF, and Lyons CR

Subjects

Base Sequence, Gene Deletion, Gene Transfer, Horizontal, Genetic Variation, Humans, Molecular Sequence Data, Mycobacterium growth & development, Open Reading Frames genetics, Sequence Analysis, DNA, DNA Transposable Elements genetics, Mycobacterium genetics, Polymorphism, Genetic

Abstract

A polymorphic region was discovered in the genetically uncharacterized opportunistic pathogen Mycobacterium abscessus. The region contains a novel 1.7 kb insertion sequence (IS) named ISMab1. ISMab1 contains two complete ORFs and one partial ORF located in segments with over 80% nucleotide identity to Mycobacterium avium IS1601 and IS999 and to previously unreported IS-like elements from Mycobacterium smegmatis. The marked similarity within this family of elements is supportive of horizontal transfer between environmental mycobacterial species. In clinical isolates, ISMab1 was either present as a single copy or absent. The polymorphic region containing ISMab1 was identified by genomic subtraction between a parental strain and phenotypic variant. The variant has a 14.2 kb genomic deletion and this is flanked in the parental strain by complex arrays of inverted and direct repeats. Clinical isolates of M. abscessus were probed for the deletion and flanking sequences and two were found to be missing more than 20 kb. No regional deletions were found in the type strain, ATCC 19977. Although M. abscessus is a rapidly growing species, comparative sequence analysis of 23 kb from the polymorphic region showed that most local ORFs have greater amino acid identity to proteins encoded by genes from the slowly growing mycobacteria, M. avium and Mycobacterium tuberculosis, than to the rapid-grower M. smegmatis. Several ORFs also have strong similarity to Pseudomonas aeruginosa genes with a potential role in beta-oxidation.

Published

2002

48. Genetic vaccines protect against Sin Nombre hantavirus challenge in the deer mouse (Peromyscus maniculatus).

Author

Bharadwaj M, Mirowsky K, Ye C, Botten J, Masten B, Yee J, Lyons CR, and Hjelle B

Subjects

Animals, Antibodies, Viral blood, DNA, Complementary, Hantavirus Infections immunology, Injections, Intramuscular, Mice, Nucleocapsid genetics, Nucleocapsid immunology, Peromyscus, Sin Nombre virus genetics, Spleen cytology, Spleen immunology, Viral Envelope Proteins genetics, Viral Envelope Proteins immunology, Hantavirus Infections prevention & control, Sin Nombre virus immunology, Vaccines, DNA administration & dosage, Viral Vaccines administration & dosage

Abstract

We used a deer mouse (Peromyscus maniculatus) infection model to test the protective efficacy of genetic vaccine candidates for Sin Nombre (SN) virus that were known to provoke immunological responses in BALB/c mice (Bharadwaj et al., Vaccine 17, 2836-2843, 1999 ). Protective epitopes were localized in each of four overlapping cDNA fragments that encoded portions of the SN virus G1 glycoprotein antigen; the nucleocapsid gene also was protective. The protective efficacy of glycoprotein gene fragments correlated with splenocyte proliferation in the presence of cognate antigen, but none induced neutralizing antibodies. Genetic vaccines against SN virus can protect outbred deer mice from infection even in the absence of a neutralizing antibody response.

Published

2002

49. Ultraviolet light induces reactivation in a murine model of cutaneous herpes simplex virus-1 infection.

Author

Goade DE, Nofchissey RA, Kusewitt DF, Hjelle B, Kreisel J, Moore J, and Lyons CR

Subjects

Animals, Female, Herpes Simplex pathology, Herpesvirus 1, Human pathogenicity, Herpesvirus 1, Human radiation effects, Male, Mice, Mice, Hairless, Photobiology, Recurrence, Ultraviolet Rays adverse effects, Herpes Simplex etiology

Abstract

We have developed a model of cutaneous herpes simplex virus-1 (HSV-1) reactivation in SKH-1 hairless mice which closely mimics the condition in humans. Sixty plaque-forming units of HSV-1 strain 17 syn+ were applied to a superficially abraded area on the lateral body wall. More than 85% of mice developed primary HSV-1 infection characterized by a zosteriform pattern of cutaneous vesiculation and ulceration. Approximately one-third of mice with primary skin lesions succumbed to neurologic disease and in the remaining mice cutaneous lesions healed completely. Subsequent exposure of healed areas to two minimal inflammatory doses of UV resulted in recrudescence of skin lesions in the irradiated areas in almost 60% of mice. Lesions appeared approximately 4 days after irradiation, persisted for 3-5 days and then resolved completely. Reactivation rarely resulted in death due to neurologic disease. Primary lesions had a histologic appearance typical of cutaneous HSV-1 infection with vesicles and focal epithelial necrosis accompanied by the formation of epithelial syncytial cells and the presence of herpetic intranuclear inclusion bodies. In primary lesions HSV-1 was demonstrated by immunohistochemistry, polymerase chain reaction and culture. In reactivated lesions epithelial syncytia and inclusion bodies were not seen; however, virus was demonstrable by polymerase chain reaction and culture. Exposure of the uninfected side to UV did not stimulate disease recurrence suggesting that local effects of UV rather than systemic immunosuppression were responsible for reactivation. Reactivation could also be obtained with two minimal inflammatory doses of UV from a UV-340 light source which emits light approximating the solar spectrum.

Published

2001

50. Ovalbumin aerosols induce airway hyperreactivity in naïve DO11.10 T cell receptor transgenic mice without pulmonary eosinophilia or OVA-specific antibody.

Author

Wilder JA, Collie DD, Bice DE, Tesfaigzi Y, Lyons CR, and Lipscomb MF

Subjects

Administration, Intranasal, Aerosols, Airway Resistance, Animals, Cytokines analysis, Eosinophilia, Female, Immunization, Immunization Schedule, Immunoglobulin E blood, Immunoglobulin G blood, Immunophenotyping, Lung pathology, Lymphocyte Activation, Male, Mice, Mice, Inbred BALB C, Mice, Knockout, Mice, Transgenic, Models, Animal, Ovalbumin administration & dosage, Receptors, Antigen, T-Cell, alpha-beta deficiency, Receptors, Antigen, T-Cell, alpha-beta genetics, Specific Pathogen-Free Organisms, Bronchial Hyperreactivity chemically induced, Ovalbumin toxicity, Receptors, Antigen, T-Cell, alpha-beta immunology

Abstract

The pathobiology of allergic asthma is being studied using murine models, most of which use systemic priming followed by pulmonary challenges with the immunizing antigen. In general, mice develop eosinophilic pulmonary inflammation, increased antigen-specific immunoglobulins, and airway hyperreactivity (AHR), all of which are dependent on antigen-specific T cell activation. To establish a model of allergic asthma, which did not require systemic priming, we exposed DO11.10 T cell receptor transgenic mice, which have an expanded repertoire of ovalbumin (OVA), peptide-specific T cells, to limited aerosols of OVA protein. DO11.10 +/- mice developed AHR in the absence of increases in total serum IgE, OVA-specific IgG, or eosinophilia. The AHR was accompanied by pulmonary recruitment of antigen-specific T cells with decreased expression of CD62L and CD45RB and increased expression of CD69, a phenotype indicative of T cell activation. Our results support recent hypotheses that T cells mediate AHR directly.

Published

2001