Efficacy of Primate Humoral Passive Transfer in a Murine Model of Pneumonic Plague Is Mouse Strain-Dependent

被引:5
|
作者
Graham, V. A. [1 ]
Hatch, G. J. [1 ]
Bewley, K. R. [1 ]
Steeds, K. [1 ]
Lansley, A. [1 ]
Bate, S. R. [1 ]
Funnell, S. G. P. [1 ]
机构
[1] Publ Hlth England, Microbiol Serv, Salisbury SP4 0JG, Wilts, England
关键词
YERSINIA-PESTIS; SUBUNIT VACCINE; MONOCLONAL-ANTIBODIES; V-ANTIGENS; PROTECTION; MICE; PROTEIN; F1; IMMUNIZATION; RESISTANCE;
D O I
10.1155/2014/807564
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
New vaccines against biodefense-related and emerging pathogens are being prepared for licensure using the US Federal Drug Administration's "Animal Rule." This allows licensure of drugs and vaccines using protection data generated in animal models. A new acellular plague vaccine composed of two separate recombinant proteins (rF1 and rV) has been developed and assessed for immunogenicity in humans. Using serum obtained from human volunteers immunised with various doses of this vaccine and from immunised cynomolgus macaques, we assessed the pharmacokinetic properties of human and cynomolgus macaque IgG in BALB/c and the NIH Swiss derived Hsd:NIHS mice, respectively. Using human and cynomolgus macaque serum with known ELISA antibody titres against both vaccine components, we have shown that passive immunisation of human and nonhuman primate serum provides a reproducible delay in median time to death in mice exposed to a lethal aerosol of plague. In addition, we have shown that Hsd: NIHS mice are a better model for humoral passive transfer studies than BALB/c mice.
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页数:11
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