Your search keyword '"Anthrax mortality"' showing total 6 results

1. Evaluation of liposomal ciprofloxacin formulations in a murine model of anthrax.

Author

Stratilo CW, Jager S, Crichton M, and Blanchard JD

Subjects

Administration, Intranasal, Animals, Anthrax microbiology, Anthrax mortality, Bacillus anthracis pathogenicity, Ciprofloxacin chemistry, Disease Models, Animal, Drug Compounding, Female, Mice, Mice, Inbred BALB C, Survival Rate, Anthrax drug therapy, Ciprofloxacin therapeutic use, Liposomes chemistry

Abstract

The in vivo efficacy of liposomal encapsulated ciprofloxacin in two formulations, lipoquin and apulmiq, were evaluated against the causative agent of anthrax, Bacillus anthracis. Liposomal encapsulated ciprofloxacin is attractive as a therapy since it allows for once daily dosing and achieves higher concentrations of the antibiotic at the site of initial mucosal entry but lower systemic drug concentrations. The in vivo efficacy of lipoquin and apulmiq delivered by intranasal instillation was studied at different doses and schedules in both a post exposure prophylaxis (PEP) therapy model and in a delayed treatment model of murine inhalational anthrax. In the mouse model of infection, the survival curves for all treatment cohorts differed significantly from the vehicle control. Ciprofloxacin, lipoquin and apulmiq provided a high level of protection (87-90%) after 7 days of therapy when administered within 24 hours of exposure. Reducing therapy to only three days still provided protection of 60-87%, if therapy was provided within 24 hours of exposure. If treatment was initiated 48 hours after exposure the survival rate was reduced to 46-65%. These studies suggest that lipoquin and apulmiq may be attractive therapies as PEP and as part of a treatment cocktail for B. anthracis., Competing Interests: J. B. is an employee of Aradigm Corp and has been named on Aradigm patents. C.W.S., M.C. and S.J. declare no potential conflict of interest. This does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published

2020

2. A systematic review and meta-analysis of preclinical trials testing anti-toxin therapies for B. anthracis infection: A need for more robust study designs and results.

Author

Xu W, Ohanjanian L, Sun J, Cui X, Suffredini D, Li Y, Welsh J, and Eichacker PQ

Subjects

Animals, Anthrax mortality, Disease Models, Animal, Humans, Research Design, Treatment Outcome, Anthrax drug therapy, Anti-Bacterial Agents therapeutic use, Antigens, Bacterial therapeutic use, Antitoxins therapeutic use, Bacillus anthracis

Abstract

Background: B. anthracis anti-toxin agents are approved and included in the Strategic National Stockpile based primarily on animal infection trials. However, in the only anthrax outbreak an approved anti-toxin agent was administered in, survival did not differ comparing recipients and non-recipients, although recipients appeared sicker., Objective: Employ a systematic review and meta-analysis to investigate preclinical studies supporting anthrax anti-toxin agents., Data Source: PubMed, EMBASE, and Scopus., Study Eligibility: Compared survival with an anti-toxin agent versus control in B. anthracis challenged, antibiotic treated animals., Study Methods: Examine model and study design and the effect of anti-toxin agents on relative risk of death(95%CI) (RR)., Results: From 9 studies, 29 experiments were analyzed which included 4 species (748 animals) and 5 agents; LFI, AIG, AVP-21D9, Raxibacumab, and ETI-204. Only five experiments were blinded and no experiment included the cardiopulmonary support sick B. anthracis patients receive. Only one agent in a single un-blinded experiment reduced RR significantly [0.45(0.22,0.940]. However, in six studies testing an agent in more than one experiment in the same species, agents had consistent survival effects across experiments [I2 = 0, p≥0.55 in five and I2 = 42%, p = 0.16 in one]. Within each species, agents had effects on the side of benefit; in one study testing AVP-21D9 in mice [0.11(0.01,1.82)] or guinea pigs [0.70(0.48,1.03)]; across eight rabbit studies testing LFI, Raxibacumab, AIG or ETI-204 [0.62(0.45,0.87); I2 = 17.4%, p = 0.29]; and across three monkey studies testing Raxibacumab, AIG or ETI-204 [0.66(0.34,1.27); I2 = 25.3%, p = 0.26]. Across all agents and species, agents decreased RR [0.64(0.52,0.79); I2 = 5.3%, p = 0.39]., Limitations: Incidence of selective reporting not identifiable., Conclusions: Although overall significant, individually anti-toxin agents had weak beneficial effects. Lack of study blinding and relevant clinical therapies further weakened studies. Although difficult, preclinical studies with more robust designs and results are warranted to justify the resources necessary to maintain anti-toxin agents in national stockpiles.

Published

2017

3. Reverse-Phase Microarray Analysis Reveals Novel Targets in Lymph Nodes of Bacillus anthracis Spore-Challenged Mice.

Author

Popova TG, Espina V, Liotta LA, and Popov SG

Subjects

Animals, Anthrax mortality, Biomarkers, Disease Models, Animal, Immunohistochemistry, Lymph Nodes microbiology, Lymph Nodes pathology, Mice, Phosphoproteins metabolism, Proteome, Proteomics methods, Signal Transduction, Spores, Bacterial, Anthrax metabolism, Anthrax microbiology, Bacillus anthracis physiology, Lymph Nodes metabolism, Protein Array Analysis

Abstract

Anthrax is a frequently fatal infection of many animal species and men. The causative agent Bacillus anthracis propagates through the lymphatic system of the infected host; however, the specific interactions of the host and microbe within the lymphatics are incompletely understood. We report the first description of the phosphoprotein signaling in the lymph nodes of DBA/2 mice using a novel technique combining the reverse-phase microarray with the laser capture microdissection. Mice were challenged into foot pads with spores of toxinogenic, unencapsulated Sterne strain. The spores quickly migrated to the regional popliteal lymph nodes and spread to the bloodstream as early as 3 h post challenge. All mice died before 72 h post challenge from the systemic disease accompanied by a widespread LN tissue damage by bacteria, including the hemorrhagic necrotizing lymphadenitis, infiltration of CD11b+ and CD3+ cells, and massive proliferation of bacteria in lymph nodes. A macrophage scavenger receptor CD68/macrosialin was upregulated and found in association with vegetative bacteria likely as a marker of their prior interaction with macrophages. The major signaling findings among the 65 tested proteins included the reduced MAPK signaling, upregulation of STAT transcriptional factors, and altered abundance of a number of pro- and anti-apoptotic proteins with signaling properties opposing each other. Downregulation of ERK1/2 was associated with the response of CD11b+ macrophages/dendritic cells, while upregulation of the pro-apoptotic Puma indicated a targeting of CD3+ T-cells. A robust upregulation of the anti-apoptotic survivin was unexpected because generally it is not observed in adult tissues. Taken together with the activation of STATs it may reflect a new pathogenic mechanism aimed to delay the onset of apoptosis. Our data emphasize a notion that the net biological outcome of disease is determined by a cumulative impact of factors representing the microbial insult and the protective capacity of the host.

Published

2015

4. Combination therapy with antibiotics and anthrax immune globulin intravenous (AIGIV) is potentially more effective than antibiotics alone in rabbit model of inhalational anthrax.

Author

Kammanadiminti S, Patnaikuni RK, Comer J, Meister G, Sinclair C, and Kodihalli S

Subjects

Animals, Anthrax immunology, Anthrax mortality, Antigens, Bacterial blood, Antigens, Bacterial immunology, Bacillus anthracis immunology, Bacteremia therapy, Disease Models, Animal, Drug Therapy, Combination, Female, Levofloxacin therapeutic use, Male, Rabbits, Respiratory Tract Infections immunology, Respiratory Tract Infections mortality, Toxemia therapy, Treatment Outcome, Anthrax therapy, Anti-Bacterial Agents therapeutic use, Immunoglobulins, Intravenous therapeutic use, Respiratory Tract Infections therapy

Abstract

Background: We have evaluated the therapeutic efficacy of AIGIV when given in combination with levofloxacin and the effective window of treatment to assess the added benefit provided by AIGIV over standard antibiotic treatment alone in a New Zealand white rabbit model of inhalational anthrax., Methods: Rabbits were exposed to lethal dose of aerosolized spores of Bacillus anthracis (Ames strain) and treated intravenously with either placebo, (normal immune globulin intravenous, IGIV) or 15 U/kg of AIGIV, along with oral levofloxacin treatment at various time points (30-96 hours) after anthrax exposure., Results: The majority of treated animals (>88%) survived in both treatment groups when treatment was initiated within 60 hours of post-exposure. However, reduced survival of 55%, 33% and 25% was observed for placebo + levofloxacin group when the treatment was initiated at 72, 84 and 96 hours post-exposure, respectively. Conversely, a survival rate of 65%, 40% and 71% was observed in the AIGIV + levofloxacin treated groups at these time points., Conclusions: The combination of AIGIV with antibiotics provided an improvement in survival compared to levofloxacin treatment alone when treatment was delayed up to 96 hours post-anthrax exposure. Additionally, AIGIV treatment when given as an adjunct therapy at any of the time points tested did not interfere with the efficacy of levofloxacin.

Published

2014

5. Lethality in a murine model of pulmonary anthrax is reduced by combining nuclear transport modifier with antimicrobial therapy.

Author

Veach RA, Zienkiewicz J, Collins RD, and Hawiger J

Subjects

Active Transport, Cell Nucleus drug effects, Animals, Anthrax complications, Anthrax pathology, Anti-Infective Agents pharmacology, Cell-Penetrating Peptides administration & dosage, Cell-Penetrating Peptides pharmacology, Ciprofloxacin administration & dosage, Ciprofloxacin pharmacology, Cytokines blood, Cytokines metabolism, Disease Models, Animal, Drug Combinations, Female, Lung Diseases etiology, Lung Diseases pathology, Membrane Proteins administration & dosage, Membrane Proteins pharmacology, Mice, Peptides, Cyclic administration & dosage, Peptides, Cyclic pharmacology, Survival Analysis, Treatment Outcome, Anthrax drug therapy, Anthrax mortality, Anti-Infective Agents administration & dosage, Lung Diseases drug therapy, Lung Diseases mortality

Abstract

Background: In the last ten years, bioterrorism has become a serious threat and challenge to public health worldwide. Pulmonary anthrax caused by airborne Bacillus anthracis spores is a life-threatening disease often refractory to antimicrobial therapy. Inhaled spores germinate into vegetative forms that elaborate an anti-phagocytic capsule along with potent exotoxins which disrupt the signaling pathways governing the innate and adaptive immune responses and cause endothelial cell dysfunction leading to vascular injury in the lung, hypoxia, hemorrhage, and death., Methods/principal Findings: Using a murine model of pulmonary anthrax disease, we showed that a nuclear transport modifier restored markers of the innate immune response in spore-infected animals. An 8-day protocol of single-dose ciprofloxacin had no significant effect on mortality (4% survival) of A/J mice lethally infected with B. anthracis Sterne. Strikingly, mice were much more likely to survive infection (52% survival) when treated with ciprofloxacin and a cell-penetrating peptide modifier of host nuclear transport, termed cSN50. In B. anthracis-infected animals treated with antibiotic alone, we detected a muted innate immune response manifested by cytokines, tumor necrosis factor alpha (TNFα), interleukin (IL)-6, and chemokine monocyte chemoattractant protein-1 (MCP-1), while the hypoxia biomarker, erythropoietin (EPO), was greatly elevated. In contrast, cSN50-treated mice receiving ciprofloxacin demonstrated a restored innate immune responsiveness and reduced EPO level. Consistent with this improvement of innate immunity response and suppression of hypoxia biomarker, surviving mice in the combination treatment group displayed minimal histopathologic signs of vascular injury and a marked reduction of anthrax bacilli in the lungs., Conclusions: We demonstrate, for the first time, that regulating nuclear transport with a cell-penetrating modifier provides a cytoprotective effect, which enables the host's immune system to reduce its susceptibility to lethal B. anthracis infection. Thus, by combining a nuclear transport modifier with antimicrobial therapy we offer a novel adjunctive measure to control florid pulmonary anthrax disease.

Published

2012

6. Exogenous interferon-alpha and interferon-gamma increase lethality of murine inhalational anthrax.

Author

Gold JA, Hoshino Y, Jones MB, Hoshino S, Nolan A, and Weiden MD

Subjects

Administration, Inhalation, Animals, Female, Humans, Interleukins blood, Interleukins immunology, Lung immunology, Lung microbiology, MAP Kinase Kinase 3 genetics, MAP Kinase Kinase 3 metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, STAT1 Transcription Factor genetics, STAT1 Transcription Factor immunology, Signal Transduction physiology, Spleen immunology, Spleen microbiology, Spores, Bacterial immunology, Survival Rate, Anthrax immunology, Anthrax mortality, Bacillus anthracis immunology, Bacillus anthracis pathogenicity, Interferon-alpha immunology, Interferon-gamma immunology

Abstract

Background: Bacillus anthracis, the etiologic agent of inhalational anthrax, is a facultative intracellular pathogen. Despite appropriate antimicrobial therapy, the mortality from inhalational anthrax approaches 45%, underscoring the need for better adjuvant therapies. The variable latency between exposure and development of disease suggests an important role for the host's innate immune response. Type I and Type II Interferons (IFN) are prominent members of the host innate immune response and are required for control of intracellular pathogens. We have previously described a protective role for exogenous Type I and Type II IFNs in attenuating intracellular B.anthracis germination and macrophage cell death in vitro., Methodology and Principal Findings: We sought to extend these findings in an in vivo model of inhalational anthrax, utilizing the Sterne strain (34F2) of B.anthracis. Mice devoid of STAT1, a component of IFN-alpha and IFN-gamma signaling, had a trend towards increased mortality, bacterial germination and extrapulmonary spread of B.anthracis at 24 hrs. This was associated with impaired IL-6, IL-10 and IL-12 production. However, administration of exogenous IFN-gamma, and to a lesser extent IFN-alpha, at the time of infection, markedly increased lethality. While IFNs were able to reduce the fraction of germinated spores within the lung, they increased both the local and systemic inflammatory response manifest by increases in IL-12 and reductions in IL-10. This was associated with an increase in extrapulmonary dissemination. The mechanism of IFN mediated inflammation appears to be in part due to STAT1 independent signaling., Conclusions: In conclusion, while endogenous IFNs are essential for control of B.anthracis germination and lethality, administration of exogenous IFNs appear to increase the local inflammatory response, thereby increasing mortality.

Published

2007