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Open AccessJournal ArticleDOI

Interferon-gamma is crucial for surviving a Brucella abortus infection in both resistant C57BL/6 and susceptible BALB/c mice.

TLDR
Gen knock‐out mice were utilized to elucidate some of the salient components of resistance to Brucella abortus and death in both strains of IFN‐γ gene disrupted mice coincided with symptoms of cachexia and macrophages comprised ≥ 75% of the splenic leucocytes.
Abstract
Brucella abortus is an intracellular bacterial pathogen that causes chronic infections in humans and a number of agriculturally important species of animals. It has been shown that BALB/c mice are more susceptible to infections with virulent strains of Brucella abortus than C57BL/6 or C57BL/10 strains. In experiments described here, gene knock-out mice were utilized to elucidate some of the salient components of resistance. Resistant C57BL/6 mice with gene deletions or disruptions in the interferon-gamma (IFN-gamma), perforin or beta(2)-microglobulin genes had decreased abilities to control intracellular infections with B. abortus strain 2308 during the first week after infection. However, only the IFN-gamma knock-out mice had a sustained inability to control infections and this resulted in death of the mice at approximately 6 weeks post-infection. These mice had a continual increase in the number of bacterial colony-forming units (CFU) in their spleens until death. When BALB/c mice with the disrupted IFN-gamma gene were infected they had more splenic CFU at one week post-infection than control mice but the increase was not statistically significant and by 3 weeks they did not have more CFU than control mice. Moreover, the number of splenic bacteria did not increase in the BALB/c IFN-gamma knock-out mice between 6 and 10.5 weeks, although they died at 10.5 weeks, the time by which normal BALB/c mice were clearing the infection. Death in both strains of IFN-gamma gene disrupted mice coincided with symptoms of cachexia and macrophages comprised > or= 75% of the splenic leucocytes.

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Brucellosis vaccines: past, present and future.

TL;DR: Attempts are being made to develop defined rough mutant vaccine strains that would be more effective against B. melitensis and B. suis, with or without adjuvants.
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Molecular Host-Pathogen Interaction in Brucellosis: Current Understanding and Future Approaches to Vaccine Development for Mice and Humans

TL;DR: The current understanding of Brucella pathogenesis and host immunity for the development of genetically defined efficient vaccine strains are provided and conditions required for an effective BrucellA vaccine strain are postulated.
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Brucella intracellular life: from invasion to intracellular replication.

TL;DR: The integrity of BrucellA LPS on the bacterial surface is one of the required factors for Brucella intracellular survival, and therefore for virulence.
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Interactions of the Human Pathogenic Brucella Species with Their Hosts

TL;DR: Recent insights into mechanisms of intracellular survival and immune evasion that contribute to systemic persistence by the pathogenic Brucella species are discussed.
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What have we learned from brucellosis in the mouse model

TL;DR: It is concluded that, when used properly, the mouse is a valuable brucellosis model and a useful virulence/attenuation index and is used in vaccine (Residual Virulence) quality control.
References
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Journal Article

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Temporal development of protective cell-mediated and humoral immunity in BALB/c mice infected with Brucella abortus.

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Endogenous gamma interferon mediates resistance to Brucella abortus infection.

TL;DR: The results indicated that endogenous IFN-gamma plays an important role in mediating resistance to primary and secondary Brucella infection.
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