Literature DB >> 9125557

Gamma interferon is not essential in host defense against disseminated candidiasis in mice.

Q Qian1, J E Cutler.   

Abstract

In vitro studies have suggested a role for interferon gamma (IFN-gamma) in host defense against disseminated candidiasis, but in vivo studies are inconclusive. We utilized homozygous IFN-gamma knockout (GKO) mice to determine if the cytokine is essential in host defense against this disease. Genotypes of mice were determined by PCR with specific primers for the normal or disrupted IFN-gamma gene. The GKO status of the mice was confirmed by an enzyme-linked immunosorbent assay, which showed no detectable IFN-gamma produced by their splenocytes stimulated by concanavalin A. To test the susceptibility of GKO mice to candidiasis, the animals were infected either intravenously (i.v.) or intragastrically (i.g.) with Candida albicans. GKO mice infected i.v. survived as long as wild-type (WT) mice and showed no difference in Candida CFU counts in liver, spleen, or kidneys compared to those for WT mice. When animals were given Candida i.g., at 3 h or at 10 or 21 days after infection, there was no dissemination of Candida to the lung, liver, spleen, or kidneys for either GKO or WT mice. There was no difference in Candida CFU counts recovered from the stomach or intestines between GKO and WT mice. Histological examination of the stomach cardial-atrium fold, where the fungus was located, showed that GKO mice did not have evidence of more tissue damage or fungal invasion than WT mice. Finally, the jejunum for both types of mice showed no evidence of tissue damage or fungal invasion. These studies indicate that IFN-gamma is not essential in host defense against C. albicans that originates from a mucosal site or that is given directly into the bloodstream in a mouse model.

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Year:  1997        PMID: 9125557      PMCID: PMC175210          DOI: 10.1128/iai.65.5.1748-1753.1997

Source DB:  PubMed          Journal:  Infect Immun        ISSN: 0019-9567            Impact factor:   3.441


  54 in total

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Authors:  J E Cutler; D L Brawner; K C Hazen; M A Jutila
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Authors:  R K Li; J E Cutler
Journal:  J Gen Microbiol       Date:  1991-03

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Journal:  Infect Immun       Date:  1993-08       Impact factor: 3.441

7.  Differential adherence of hydrophobic and hydrophilic Candida albicans yeast cells to mouse tissues.

Authors:  K C Hazen; D L Brawner; M H Riesselman; M A Jutila; J E Cutler
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8.  Hepatosplenic candidiasis in children with acute leukemia.

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9.  T cell subsets and IFN-gamma production in resistance to systemic candidosis in immunized mice.

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Journal:  J Immunol       Date:  1990-06-01       Impact factor: 5.422

10.  Application of DNA typing methods to Candida albicans epidemiology and correlations with phenotype.

Authors:  D A Stevens; F C Odds; S Scherer
Journal:  Rev Infect Dis       Date:  1990 Mar-Apr
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4.  Candida albicans killing by RAW 264.7 mouse macrophage cells: effects of Candida genotype, infection ratios, and gamma interferon treatment.

Authors:  A Marcil; D Harcus; D Y Thomas; M Whiteway
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Journal:  Antimicrob Agents Chemother       Date:  2002-05       Impact factor: 5.191

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Review 8.  IL-12 and related cytokines: function and regulatory implications in Candida albicans infection.

Authors:  Robert B Ashman; Dipti Vijayan; Christine A Wells
Journal:  Clin Dev Immunol       Date:  2010-11-01

9.  Role for endosomal and vacuolar GTPases in Candida albicans pathogenesis.

Authors:  Douglas A Johnston; Karen E Eberle; Joy E Sturtevant; Glen E Palmer
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10.  Commensal enteric bacteria lipopolysaccharide impairs host defense against disseminated Candida albicans fungal infection.

Authors:  T T Jiang; V Chaturvedi; J M Ertelt; L Xin; D R Clark; J M Kinder; S S Way
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  10 in total

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