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1 Department of Obstetrics and Gynecology, 2 Anatomy and Neuroscience, and 3 Microbiology and Immunology, The University of Texas Medical Branch, Galveston, Texas 77555 - 1062
Previous studies have
demonstrated that nitric oxide (NO) is involved in the uterine host
defense against bacterial infection. In nonpregnant rats, NO
production in the uterus was shown to be lower, and inducible NO
synthase (NOS) expression was undetectable. However, studies in
pregnant rats show abundant expression of inducible NOS with
significant elevation in NO production in the uterus. We have recently
reported that intrauterine Escherichia coli infection caused
a localized increase in uterine NO production and inducible NOS
expression in the nonpregnant rat. In our present study, we examined
whether the uterine NO production, NOS expression, and uterine tumor
necrosis factor-
protein are increased in pregnant rats with
intrauterine pathogenic Escherichia coli infection. Unlike
the nonpregnant state, the NO production in the infected uterine horn
of pregnant rats was not significantly elevated after bacterial
inoculation compared with the contralateral uterine horn. The
expression of uterine NOS (types II and III) also did not show
significant upregulation in the infected horn. This is in contrast to
that in nonpregnant animals, in which type II NOS was induced in the
uterus on infection. Moreover, intrauterine infection induced an
elevated expression of tumor necrosis factor- protein in the
infected horn both of nonpregnant and of pregnant rats. These data
suggest that the sequential stimulation of NOS expression, especially
the inducible isoform, and generation of uterine NO are lacking during
pregnancy despite an elevated tumor necrosis factor- after
infection. In summary, NO synthesis response may be maximal at
pregnancy, and infection may not further induce the NO system. Present
studies, together with our previous report that intrauterine
infection-induced lethality in pregnancy rats was amplified with the
inhibition of NO, suggest that pregnancy is a state predisposed for
increased complications associated with intrauterine infection and that
the constitutively elevated uterine NO during pregnancy may help
contain or even reduce the risk of infection-related complications.
cytokines; Escherichia coli; gestation; Dr fimbriae; nitric oxide
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