4.6 Article

Cryptococcal Urease Promotes the Accumulation of Immature Dendritic Cells and a Non-Protective T2 Immune Response within the Lung

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AMERICAN JOURNAL OF PATHOLOGY
卷 174, 期 3, 页码 932-943

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ELSEVIER SCIENCE INC
DOI: 10.2353/ajpath.2009.080673

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资金

  1. Merit Review awards
  2. Career Development Award
  3. Research Enhancement Award Program
  4. Department of Veterans Affairs
  5. National Institutes of Health [T32-HL07749, R01-HL63670, R01-HL65912, R01-HL51082, R01-HL082480, R01-HL056309]
  6. Burroughs Wellcome Fund

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Urease, a major virulence factor for Cryptococcus neoformans, promotes lethal meningitis/encephalitis in mice. The effect of urease within the lung, the primary site of most invasive fungal infections, is unknown. An established model of murine infection that utilizes either urease-producing (wt and ure1::URE1) or urease-deficient (ure1) strains (H99) of C neoformans was used to characterize fungal clearance and the resultant immune response evoked by these strains within the lung. Results indicate that mice infected with urease-producing strains of C neoformans demonstrate a 100-fold increase in fungal burden beginning 2 weeks post-infection (as compared with mice infected with urease-deficient organisms). Infection with urease-producing C neoformans was associated with a highly polarized T2 immune response as evidenced by increases in the following: 1) pulmonary eosinophils, 2) serum IgE levels, 3) T2 cytokines (interleukin-4, -13, and -4 to interferon-gamma ratio), and 4) alternatively activated macrophages. Furthermore, the percentage and total numbers of immature dendritic cells within the lung-associated lymph nodes was markedly increased in mice infected with urease-producing C neoformans. Collectively, these data define cryptococcal urease as a pulmonary virulence factor that promotes immature dendritic cell accumulation and a potent, yet non-protective, T2 immune response. These findings provide new insights into mechanisms by which microbial factors contribute to the immunopathology associated with invasive fungal disease. (Am J Pathol 2009, 174:932-943; DOI: 10.2353/ajpath.2009.080673)

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