The Journal of Medical Microbiology, Vol 44, Issue 6 490-495, Copyright © 1996 by Society for General Microbiology
Streptococcus pneumoniae in the nasal cavity of mice causes lower respiratory tract infection after airway obstruction
Y. Iizawa, N. Kitamoto, K. Hiroe and M. Nakao
Pharmaceutical Research Laboratories III, Pharmaceutical Research Division, Takeda Chemical Industries Ltd, Osaka, Japan.
A model of persistent colonisation in the nasal cavity of mice by
Streptococcus pneumoniae has been established. S. pneumoniae NNP-4 was
introduced to the lungs of CBA/J mice at a density of c. 10(4) cfu/lung by
an aerosol method and a high dose of ampicillin was administered 1 h after
infection. This antibiotic eliminated bacteria from the lungs and trachea,
but did not affect the bacterial counts in the nasal cavity. In mice given
ampicillin, the bacteria were recovered from the nasal cavity only more
than 2 weeks after infection, but IgG antibody against the colonising
organisms was produced in sera around day 8 after infection. Airway
obstruction was induced by intratracheal injection of formalin 2% into
mice. Organisms appeared in the lungs in greater numbers when formalin was
injected before the antibody production than when the immunity was
established. In the early stages of infection, 10(3)-10(4) cfu appeared in
the lungs 6 h after the formalin injection and the bacterial counts
increased to c. 10(6) cfu within 24 h. When ampicillin was administered
again 1 h after formalin was given, no bacteria were recovered from lungs 6
h later. However, in some of the mice given ampicillin after formalin,
bacteria appeared in the lungs on the next day and the bacterial counts
increased thereafter. These results suggest that S. pneumoniae in the nasal
cavity invade the lower respiratory tract and that these organisms can
localise and proliferate in lungs in the event of damage to the airway.
