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Targeting resident memory T cell immunity culminates in pulmonary and systemic protection against Brucella infection
by
Yang, Xinghong
, Wang, Hongbin
, Hoffman, Carol
, Pascual, David W.
, Clapp, Beata
in
Administration, Mucosal
/ Animals
/ Bacterial diseases
/ Bacterial infections
/ Biology and Life Sciences
/ Brucella
/ Brucella abortus - genetics
/ Brucella abortus - immunology
/ Brucella Vaccine - administration & dosage
/ Brucella Vaccine - immunology
/ Brucellosis
/ Brucellosis - immunology
/ Brucellosis - prevention & control
/ CD103 antigen
/ CD4 antigen
/ CD44 antigen
/ CD69 antigen
/ CD8 antigen
/ CD8-Positive T-Lymphocytes - immunology
/ Depletion
/ Experiments
/ Female
/ Immunogenicity, Vaccine
/ Immunologic Memory
/ Immunological memory
/ Immunology
/ Infections
/ Infectious diseases
/ Interleukin 17
/ Laboratory animals
/ Livestock
/ Lung Diseases - immunology
/ Lung Diseases - microbiology
/ Lung Diseases - prevention & control
/ Lungs
/ Lymphocytes
/ Lymphocytes T
/ Medicine and Health Sciences
/ Memory cells
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Mucosa
/ Mutants
/ Mutation
/ Neutralization
/ Parenchyma
/ Pathogens
/ Physical Sciences
/ Research and Analysis Methods
/ Tumor necrosis factor-α
/ Vaccines
/ Vaccines, Attenuated - genetics
/ Vaccines, Attenuated - immunology
/ Viral infections
/ Zoonoses
/ γ-Interferon
2020
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Targeting resident memory T cell immunity culminates in pulmonary and systemic protection against Brucella infection
by
Yang, Xinghong
, Wang, Hongbin
, Hoffman, Carol
, Pascual, David W.
, Clapp, Beata
in
Administration, Mucosal
/ Animals
/ Bacterial diseases
/ Bacterial infections
/ Biology and Life Sciences
/ Brucella
/ Brucella abortus - genetics
/ Brucella abortus - immunology
/ Brucella Vaccine - administration & dosage
/ Brucella Vaccine - immunology
/ Brucellosis
/ Brucellosis - immunology
/ Brucellosis - prevention & control
/ CD103 antigen
/ CD4 antigen
/ CD44 antigen
/ CD69 antigen
/ CD8 antigen
/ CD8-Positive T-Lymphocytes - immunology
/ Depletion
/ Experiments
/ Female
/ Immunogenicity, Vaccine
/ Immunologic Memory
/ Immunological memory
/ Immunology
/ Infections
/ Infectious diseases
/ Interleukin 17
/ Laboratory animals
/ Livestock
/ Lung Diseases - immunology
/ Lung Diseases - microbiology
/ Lung Diseases - prevention & control
/ Lungs
/ Lymphocytes
/ Lymphocytes T
/ Medicine and Health Sciences
/ Memory cells
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Mucosa
/ Mutants
/ Mutation
/ Neutralization
/ Parenchyma
/ Pathogens
/ Physical Sciences
/ Research and Analysis Methods
/ Tumor necrosis factor-α
/ Vaccines
/ Vaccines, Attenuated - genetics
/ Vaccines, Attenuated - immunology
/ Viral infections
/ Zoonoses
/ γ-Interferon
2020
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Targeting resident memory T cell immunity culminates in pulmonary and systemic protection against Brucella infection
by
Yang, Xinghong
, Wang, Hongbin
, Hoffman, Carol
, Pascual, David W.
, Clapp, Beata
in
Administration, Mucosal
/ Animals
/ Bacterial diseases
/ Bacterial infections
/ Biology and Life Sciences
/ Brucella
/ Brucella abortus - genetics
/ Brucella abortus - immunology
/ Brucella Vaccine - administration & dosage
/ Brucella Vaccine - immunology
/ Brucellosis
/ Brucellosis - immunology
/ Brucellosis - prevention & control
/ CD103 antigen
/ CD4 antigen
/ CD44 antigen
/ CD69 antigen
/ CD8 antigen
/ CD8-Positive T-Lymphocytes - immunology
/ Depletion
/ Experiments
/ Female
/ Immunogenicity, Vaccine
/ Immunologic Memory
/ Immunological memory
/ Immunology
/ Infections
/ Infectious diseases
/ Interleukin 17
/ Laboratory animals
/ Livestock
/ Lung Diseases - immunology
/ Lung Diseases - microbiology
/ Lung Diseases - prevention & control
/ Lungs
/ Lymphocytes
/ Lymphocytes T
/ Medicine and Health Sciences
/ Memory cells
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Mucosa
/ Mutants
/ Mutation
/ Neutralization
/ Parenchyma
/ Pathogens
/ Physical Sciences
/ Research and Analysis Methods
/ Tumor necrosis factor-α
/ Vaccines
/ Vaccines, Attenuated - genetics
/ Vaccines, Attenuated - immunology
/ Viral infections
/ Zoonoses
/ γ-Interferon
2020
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Targeting resident memory T cell immunity culminates in pulmonary and systemic protection against Brucella infection
Journal Article
Targeting resident memory T cell immunity culminates in pulmonary and systemic protection against Brucella infection
2020
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Overview
Brucellosis remains the most common zoonotic disease globally. Currently no vaccines for humans exist, and conventional brucellosis vaccines for livestock fail to confer complete protection; hence, an improved vaccine is needed. Although Brucella infections primarily occur following a mucosal exposure, vaccines are administered parenterally. Few studies have considered mucosal vaccinations, or even targeting of tissue-resident memory T (TRM) cells. TRM cells protect against viral infections, but less is known of their role in bacterial infections, and even less for brucellosis. Oral prime, nasal boost with a newly developed Brucella abortus double mutant (znBAZ) confers nearly complete protection against pulmonary challenge with wild-type (wt) B. abortus 2308, and its protective efficacy is >2800-fold better than the RB51 vaccine. Vaccination with znBAZ potently stimulated CD8+ T cells, whereas mucosal vaccination with RB51 induced mostly CD4+ T cells. Subsequent analysis revealed these pulmonary CD44+ CD69+ CD8+ T cells to be either CD103+ or CD103- TRM cells, and these sequestered to the lung parenchyma as CXCR3lo and to the airways as CXCR3hi. Both CD8+ TRM subsets contained single-positive IFN-γ and TNF-α, as well as, polyfunctional cells. IL-17-producing CD8+ TRM cells were also induced by znBAZ vaccination, but in vivo IL-17 neutralization had no impact upon protection. In vivo depletion of CD4+ T cells had no impact upon protection in znBAZ-vaccinated mice. In contrast, CD4+ T cell depletion reduced RB51's protective efficacy in spleens and lungs by two- and three-logs, respectively. Although anti-CD8 mAb-treated znBAZ-vaccinated mice showed a significantly reduced pulmonary efficacy, this treatment failed to completely deplete the lung CD8+ T cells, leaving the CD103+ and CD103- CD8+ TRM cell ratios intact. Only znBAZ-vaccinated CD8-/- mice were fully sensitive to pulmonary challenge with virulent wt B. abortus 2308 since CD8+ TRM cells could not be induced. Collectively, these data demonstrate the key role of mucosal vaccination for the generation of CD8+ TRM cells in protecting against pulmonary challenge with virulent B. abortus.
Publisher
Public Library of Science,Public Library of Science (PLoS)
Subject
/ Animals
/ Brucella
/ Brucella abortus - immunology
/ Brucella Vaccine - administration & dosage
/ Brucella Vaccine - immunology
/ Brucellosis - prevention & control
/ CD8-Positive T-Lymphocytes - immunology
/ Female
/ Lung Diseases - microbiology
/ Lung Diseases - prevention & control
/ Lungs
/ Medicine and Health Sciences
/ Mucosa
/ Mutants
/ Mutation
/ Research and Analysis Methods
/ Vaccines
/ Vaccines, Attenuated - genetics
/ Vaccines, Attenuated - immunology
/ Zoonoses
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