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Vaccination with mannan protects mice against systemic aspergillosis
30
Citations
32
References
2012
Year
Microbial PathogensFungal Cell BiologyImmunodeficienciesImmunologyClinical MycologyImmunotherapeuticsSystemic AspergillosisImmune SystemImmunotherapyMg Unconjugated MannanMucosal VaccinationInvasive AspergillosisTherapeutic VaccineHumoral ImmunityImmune FunctionFungal PathogenVaccinationAntifungal AgentMedicine
Invasive aspergillosis is a major cause of mortality in immunocompromised patients and therapeutic options are often limited, thus a vaccine would be desirable. We presently studied acid-stable cell-wall mannan (α-1, 6-linked backbone highly branched with α-1, 2; α-1, 3; and β-1, 2-linked manno-oligomers) derived from C. albicans, with or without conjugation to bovine serum albumin (BSA), as a vaccine against systemic aspergillosis. Mice were vaccinated subcutaneously with mannan or mannan-BSA conjugate weekly 3 times, ending 2 weeks prior to infection with A. fumigatus conidia. Results showed that the protection induced by mannan is dose-dependent; 12 mg unconjugated mannan alone or > 0.3 mg mannan-BSA consistently enhanced survival (P < 0.05). Fungal burdens in brains and kidneys were reduced after > 0.3 mg of mannan-BSA (all P < 0.05). Mannan-induced protection was improved about 40-fold by conjugation of BSA to mannan. Mannan-BSA (500 kDa) was more protective than 40 kDa mannan-BSA. Mannan is a candidate for a cross-protective conjugate fungal vaccine.
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