Impaired Control of<i>Brucella melitensis</i>Infection in<i>Rag1</i>-Deficient Mice

Izadjoo, Mina; Polotsky, Yury; Mense, Mark G.; Bhattacharjee, Apurba K.; Paranavitana, Chrysanthi; Hadfield, Ted L.; Hoover, David L.

doi:10.1128/iai.68.9.5314-5320.2000

Cited by 34 publications

(34 citation statements)

References 32 publications

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“…Independently of the formulation employed, mice immunized with BLS and adjuvants were protected against a virulent Brucella challenge. Protection was observed at the spleen and also at the liver, an important site for the control of Brucella infection by T-and B-cell-mediated defenses (14,20). From a practical point of view, an important conclusion can be drawn from our results.…”

Section: Discussionsupporting

confidence: 50%

BrucellaLumazine Synthase Elicits a Mixed Th1-Th2 Immune Response and Reduces Infection in Mice Challenged withBrucella abortus544 Independently of the Adjuvant Formulation Used

et al. 2003

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Section: Discussionsupporting

confidence: 50%

BrucellaLumazine Synthase Elicits a Mixed Th1-Th2 Immune Response and Reduces Infection in Mice Challenged withBrucella abortus544 Independently of the Adjuvant Formulation Used

et al. 2003

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“…Mice immunized with the Omp31 DNA vaccine were significantly protected against B. ovis and B. melitensis infection. Protection was observed in the spleen and also in the liver, an important site for the control of Brucella infection (17,32). Levels of protection afforded in the spleen and the liver after B. ovis challenge were comparable to the ones achieved by the H38 control vaccine.…”

Section: Discussionmentioning

confidence: 59%

A DNA Vaccine Coding for theBrucellaOuter Membrane Protein 31 Confers Protection againstB. melitensisandB. ovisInfection by Eliciting a Specific Cytotoxic Response

et al. 2005

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“…This result is not expected or predictable on the basis of previous studies. IFN-g-and IFN regulatory factor 1-deficient mice, but not RAG-, IL-12-, or MyD88-deficient mice, succumb to primary infection by Brucella (46,55,57,60,77,78), suggesting that IFN-g can be induced at low level by MyD88/IL-12-independent pathways. Our results confirm the importance of using IL-12-inducing adjuvant in Brucella vaccination.…”

Section: Discussionmentioning

confidence: 99%

Humoral Immunity and CD4+ Th1 Cells Are Both Necessary for a Fully Protective Immune Response upon Secondary Infection with Brucella melitensis

Vitry

Mambres

Trez

et al. 2014

The Journal of Immunology

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Brucella spp are intracellular bacteria that cause brucellosis, one of the most common zoonoses in the world. Given the serious medical consequences of this disease, a safe and effective human vaccine is urgently needed. Efforts to develop this vaccine have been hampered by our lack of understanding of what constitutes a protective memory response against Brucella. In this study, we characterize the cells and signaling pathways implicated in the generation of a protective immune memory response following priming by the injection of heat-killed or live Brucella melitensis 16M. Using a panel of gene-deficient mice, we demonstrated that during a secondary recall response, both the Brucella-specific humoral response and CD4+ Th1 cells must act together to confer protective immunity in the spleen to B. melitensis infection. Humoral protective immunity is induced by the inoculation of both heat-killed and live bacteria, and its development does not require T cells, MyD88/IL-12p35 signaling pathways, or an activation-induced deaminase–mediated isotype switch. In striking contrast, the presence of memory IFN-γ–producing CD4+ Th1 cells requires the administration of live bacteria and functional MyD88/IL-12p35 pathways. In summary, our work identifies several immune markers closely associated with protective immune memory and could help to define a rational strategy to obtain an effective human vaccine against brucellosis.

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Impaired Control ofBrucella melitensisInfection inRag1-Deficient Mice

Cited by 34 publications

References 32 publications

BrucellaLumazine Synthase Elicits a Mixed Th1-Th2 Immune Response and Reduces Infection in Mice Challenged withBrucella abortus544 Independently of the Adjuvant Formulation Used

BrucellaLumazine Synthase Elicits a Mixed Th1-Th2 Immune Response and Reduces Infection in Mice Challenged withBrucella abortus544 Independently of the Adjuvant Formulation Used

A DNA Vaccine Coding for theBrucellaOuter Membrane Protein 31 Confers Protection againstB. melitensisandB. ovisInfection by Eliciting a Specific Cytotoxic Response

Humoral Immunity and CD4+ Th1 Cells Are Both Necessary for a Fully Protective Immune Response upon Secondary Infection with Brucella melitensis

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