Abstract

Aerosolization is the most dangerous route of infection by select agents. Because of difficulty in diagnosis, it would be valuable to have therapies active against a broad range of aerosolized pathogens. Remarkably, ittle is known about the pathophysiology, microbiology, and immunology associated with aerosol delivery. This is due mostly to infrastructure requirements for aerosolization experiments, the specialized equipment that is necessary, and the limited number of individuals trained in the field of aerobiology. The work proposed in this application addresses this lack of understanding by combining expertise in aerobiology, microbial pathogenesis, immunology, and gene therapy. The ultimate goal of this program is to identify commonalities or deficiencies in host responses that can be targeted by immunotherapies, treatments that would benefit an individual exposed to any number of bioterrorism agents. To address this, three different select agent bacterial pathogens have been chosen for detailed study: Francisella tularensis, Yersinia pestis, and Burkholderia pseudomallei. Each of these pathogens alters host responses, thereby enhancing their success against the host. Bolstering host responses, therefore, is an attractive strategy to mitigate morbidity and mortality by agents like these three pathogens, regardless of the actual bacterium infecting the host. To identify immunotherapies providing cross-pathogen protection against aerosol infection, we propose these specific aims:
Aim 1 : To characterize the natural history of bacterial select agents delivered by aerosol. The objective of this aim is to characterize the pathophysiology of the three bacterial pathogens aerosolized into mice.
Aim 2 : To determine shared and distinct innate and bridging immune responses to bacterial select agents. These studies will characterize the innate and bridging immune response to F. tularensis, B. pseudomallei, and Y. pestis.
Aim 3 : To manipulate early host responses as therapeutic interventions. These studies will investigate whether augmenting innate and/or bridging immune responses with Th1 or Th17 effector cytokines can bolster host resistance to F. tularensis, B. pseudomallei, and Y. pestis delivered as an aerosol.

Public Health Relevance

Biological attacks are most likely to be delivered by aerosolization because this route of infection causes severe disease. The goal of these studies is to develop therapies that are active against a broad range of pulmonary infections by biodefense agents, regardless of the etiology.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54AI057168-07
Application #
8037604
Study Section
Special Emphasis Panel (ZAI1)
Project Start
Project End
Budget Start
2010-03-01
Budget End
2011-02-28
Support Year
7
Fiscal Year
2010
Total Cost
$320,954
Indirect Cost

  Institution

Name
University of Maryland Baltimore
Department
Type
DUNS #
188435911
City
Baltimore
State
MD
Country
United States
Zip Code
21201

  Publications

Champion, Anna E; Bandara, Aloka B; Mohapatra, Nrusingh et al. (2018) Further Characterization of the Capsule-Like Complex (CLC) Produced by Francisella tularensis Subspecies tularensis: Protective Efficacy and Similarity to Outer Membrane Vesicles. Front Cell Infect Microbiol 8:182
Bridge, Dacie R; Blum, Faith C; Jang, Sungil et al. (2017) Creation and Initial Characterization of Isogenic Helicobacter pylori CagA EPIYA Variants Reveals Differential Activation of Host Cell Signaling Pathways. Sci Rep 7:11057
Kaempfer, Raymond; Popugailo, Andrey; Levy, Revital et al. (2017) Bacterial superantigen toxins induce a lethal cytokine storm by enhancing B7-2/CD28 costimulatory receptor engagement, a critical immune checkpoint. Receptors Clin Investig 4:
Molleston, Jerome M; Cherry, Sara (2017) Attacked from All Sides: RNA Decay in Antiviral Defense. Viruses 9:
Cifuentes-Muñoz, Nicolás; Sun, Weina; Ray, Greeshma et al. (2017) Mutations in the Transmembrane Domain and Cytoplasmic Tail of Hendra Virus Fusion Protein Disrupt Virus-Like-Particle Assembly. J Virol 91:
Sarute, Nicolás; Ross, Susan R (2017) New World Arenavirus Biology. Annu Rev Virol 4:141-158
Chou, Yi-Ying; Cuevas, Christian; Carocci, Margot et al. (2016) Identification and Characterization of a Novel Broad-Spectrum Virus Entry Inhibitor. J Virol 90:4494-4510
Ramachandran, Girish; Tennant, Sharon M; Boyd, Mary A et al. (2016) Functional Activity of Antibodies Directed towards Flagellin Proteins of Non-Typhoidal Salmonella. PLoS One 11:e0151875
Molleston, Jerome M; Sabin, Leah R; Moy, Ryan H et al. (2016) A conserved virus-induced cytoplasmic TRAMP-like complex recruits the exosome to target viral RNA for degradation. Genes Dev 30:1658-70
Riblett, Amber M; Blomen, Vincent A; Jae, Lucas T et al. (2016) A Haploid Genetic Screen Identifies Heparan Sulfate Proteoglycans Supporting Rift Valley Fever Virus Infection. J Virol 90:1414-23

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