2009
DOI: 10.1016/j.ajog.2008.08.038
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The adaptor protein MyD88 is essential for E coli–induced preterm delivery in mice

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Cited by 48 publications
(45 citation statements)
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“…In the absence of this protein, a reduction of placental inflammation was observed, and fetal weight was therefore not affected. Consistent with this observation, using a model of preterm delivery induced by Escherichia coli infection, Filipovich and collaborators demonstrated that MyD88-deficient mice were protected from preterm delivery induced by bacterial infection compared to WT mice (53). Notably, although the MyD88-deficient mice were able to produce TNF-␣ in response to bacterial infection, the production of this cytokine was lower than in WT mice and was correlated with delayed TRIF signaling.…”
Section: Discussionsupporting
confidence: 50%
“…In the absence of this protein, a reduction of placental inflammation was observed, and fetal weight was therefore not affected. Consistent with this observation, using a model of preterm delivery induced by Escherichia coli infection, Filipovich and collaborators demonstrated that MyD88-deficient mice were protected from preterm delivery induced by bacterial infection compared to WT mice (53). Notably, although the MyD88-deficient mice were able to produce TNF-␣ in response to bacterial infection, the production of this cytokine was lower than in WT mice and was correlated with delayed TRIF signaling.…”
Section: Discussionsupporting
confidence: 50%
“…In general, infections and infectious components trigger inflammation and preterm labor in mice; however, the type of stimuli used, as well as the timing and the dose administered, may determine the type of response generated and the tissues involved. For example, high-dose LPS delivered late in gestation (ED 14-17) induces preterm labor associated with placental and fetal inflammation (38)(39)(40), whereas heat-killed Escherichia coli induces preterm labor and uterine inflammation, without changes in placental or fetal cytokines (41,42). In contrast, infection with Ureaplasma late in gestation induces placental and fetal inflammation without preterm labor (43), whereas viral infection early in gestation (ED 8.5) triggers fetal and maternal splenic inflammation, without inducing placental inflammation or preterm labor (44).…”
Section: Discussionmentioning
confidence: 99%
“…This proportion of preterm birth is less than that observed with RU486 (46) or LPS (47)(48)(49)(50) in which preterm delivery rates approach 100% possibly because fFN does not activate luteolysis or uterine contractility. Nonetheless, our experimental findings in vitro and in vivo indicate that fFN is not only a matrix molecule but is biologically active in vivo.…”
Section: Discussionmentioning
confidence: 73%