Abstract

Our overall objective is to develop approaches for effective vaccination against pulmonary tularemia. Our strategy will involve an innovative combination of vaccine approaches that will exploit TLR/NLR agonists identified in Subproject 2 and anti-oxidant F tularensis (Ft) mutants developed in Subproject 3. During the previous funding period, we made considerable progress (see Program Overview), including the demonstration that significant protection in C57BL/6 mice against the highly virulent type A strain of Ft, SchuS4, can be induced by i.n. inoculation of FcR-targeted inactivated LVS ( Ft). This is the first case to our knowledge in which an inactivated vaccine has provided protection against Ft SchuS4. In addition, anti-oxidant mutants (AAO) of Ft were found to induce partial protection against SchuS4 in the highly sensitive C57BI/6 mouse strain. In this renewal application, we will further optimize conditions for mucosal vaccination, characterize the effects of pulmonary vaccination, and define the cellular and humoral mechanisms responsible for protective immunity against SchuS4. Specifically, we will: 1) Determine the ability of i.n. vaccination with FcR-targeted immunogens in combination with use of anti-oxidant mutants (AAO) of Ft generated in Subproject 3, and /or TLR/NLR agonists identified in Subproject 2, to maximally enhance the immune response to, and levels of protection against, mucosal (i.n.) challenge with Ft SchuS4 at challenge doses up to 20,000 CPU;2) Establish the impact of Ft LVS, AAO Ft LVS and AAO Ft SchuS4, both in live and inactivated forms, on processing and presentation by M0 and DC of non-targeted and FcRtargeted Ft antigen in the presence or absence TLR/NLR agonists;and 3) Define the effector mechanisms responsible for enhanced protection after i.n. vaccination with protective immunogens identified in Aim 1 including testing the postulate that synergy between humoral and cellular immune mechanisms is required for induction of effective protection. The roles of TLR/NLRs and ROS/RNS in both inductive and effector phases will also be examined by using genetically deficient mice and specific agonists/antagonists, in consultation with the PLs of subprojects 2 and 3. The results of subproject 1 will allow the design of new mucosal vaccination platforms for effective biodefense against infection with virulent Ft and will provide novel insight into the pulmonary immune mechanisms that are responsible for protection against respiratory tularemia.

Public Health Relevance

The results of this subproject will allow the design of new mucosal vaccination strategies for effective biodefense against infection with virulent Ft and will provide novel insight into the pulmonary immune mechanisms that are responsible for protection against respiratory tularemia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI056320-09
Application #
8698573
Study Section
Special Emphasis Panel (ZAI1-LR-M (S1))
Project Start
Project End
Budget Start
2013-08-01
Budget End
2014-07-31
Support Year
9
Fiscal Year
2013
Total Cost
$456,636
Indirect Cost
$161,479

  Institution

Name
Albany Medical College
Department
Type
DUNS #
190592162
City
Albany
State
NY
Country
United States
Zip Code
12208

  Publications

Sunagar, Raju; Kumar, Sudeep; Rosa, Sarah J et al. (2018) Differential In Vitro Cultivation of Francisella tularensis Influences Live Vaccine Protective Efficacy by Altering the Immune Response. Front Immunol 9:1594
Nagar, Abhinit; DeMarco, Richard A; Harton, Jonathan A (2018) Inflammasome and Caspase-1 Activity Characterization and Evaluation: An Imaging Flow Cytometer-Based Detection and Assessment of Inflammasome Specks and Caspase-1 Activation. J Immunol :
Drake, James R (2018) The immunobiology of ubiquitin-dependent B cell receptor functions. Mol Immunol 101:146-154
Alqahtani, Maha; Ma, Zhuo; Ketkar, Harshada et al. (2018) Characterization of a Unique Outer Membrane Protein Required for Oxidative Stress Resistance and Virulence of Francisella tularensis. J Bacteriol 200:
Steiner, Donald J; Furuya, Yoichi; Metzger, Dennis W (2018) Detrimental Influence of Alveolar Macrophages on Protective Humoral Immunity during Francisella tularensis SchuS4 Pulmonary Infection. Infect Immun 86:
Chen, Fei; Cui, Guolin; Wang, Shuxia et al. (2017) Outer membrane vesicle-associated lipase FtlA enhances cellular invasion and virulence in Francisella tularensis LVS. Emerg Microbes Infect 6:e66
Periasamy, Sivakumar; Porter, Kristen A; Atianand, Maninjay K et al. (2017) Pyrin-only protein 2 limits inflammation but improves protection against bacteria. Nat Commun 8:15564
Furuya, Yoichi; Kirimanjeswara, Girish S; Roberts, Sean et al. (2017) Defective anti-polysaccharide IgG vaccine responses in IgA deficient mice. Vaccine 35:4997-5005
Holland, Kristen M; Rosa, Sarah J; Kristjansdottir, Kolbrun et al. (2017) Differential Growth of Francisella tularensis, Which Alters Expression of Virulence Factors, Dominant Antigens, and Surface-Carbohydrate Synthases, Governs the Apparent Virulence of Ft SchuS4 to Immunized Animals. Front Microbiol 8:1158
Ma, Zhuo; Russo, Vincenzo C; Rabadi, Seham M et al. (2016) Elucidation of a mechanism of oxidative stress regulation in Francisella tularensis live vaccine strain. Mol Microbiol 101:856-78

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