Hyperactive behavior in female rats in utero ‐exposed to group B Streptococcus ‐induced inflammation

2018 ◽  
Vol 69 (1) ◽  
pp. 17-22 ◽  
Author(s):  
Marie‐Julie Allard ◽  
Marie‐Elsa Brochu ◽  
Julie D. Bergeron ◽  
Guillaume Sebire
Keyword(s):  
Group B Streptococcus ◽  
In Utero ◽  
Female Rats ◽  
Hyperactive Behavior ◽  
Group B

scholarly journals Bacterial Hyaluronidase Promotes Ascending GBS Infection and Preterm Birth

mBio ◽  
2016 ◽  
Vol 7 (3) ◽  
Author(s):  
Jay Vornhagen ◽  
Phoenicia Quach ◽  
Erica Boldenow ◽  
Sean Merillat ◽  
Christopher Whidbey ◽  
...  
Keyword(s):  
Preterm Birth ◽  
Molecular Mechanisms ◽  
Group B Streptococcus ◽  
Placental Tissue ◽  
In Utero ◽  
Hyaluronidase Activity ◽  
Healthy Women ◽  
Ascending Infection ◽  
Underlying Mechanisms ◽  
Group B

ABSTRACT Preterm birth increases the risk of adverse birth outcomes and is the leading cause of neonatal mortality. A significant cause of preterm birth is in utero infection with vaginal microorganisms. These vaginal microorganisms are often recovered from the amniotic fluid of preterm birth cases. A vaginal microorganism frequently associated with preterm birth is group B streptococcus (GBS), or Streptococcus agalactiae . However, the molecular mechanisms underlying GBS ascension are poorly understood. Here, we describe the role of the GBS hyaluronidase in ascending infection and preterm birth. We show that clinical GBS strains associated with preterm labor or neonatal infections have increased hyaluronidase activity compared to commensal strains obtained from rectovaginal swabs of healthy women. Using a murine model of ascending infection, we show that hyaluronidase activity was associated with increased ascending GBS infection, preterm birth, and fetal demise. Interestingly, hyaluronidase activity reduced uterine inflammation but did not impact placental or fetal inflammation. Our study shows that hyaluronidase activity enables GBS to subvert uterine immune responses, leading to increased rates of ascending infection and preterm birth. These findings have important implications for the development of therapies to prevent in utero infection and preterm birth. IMPORTANCE GBS are a family of bacteria that frequently colonize the vagina of pregnant women. In some cases, GBS ascend from the vagina into the uterine space, leading to fetal injury and preterm birth. Unfortunately, little is known about the mechanisms underlying ascending GBS infection. In this study, we show that a GBS virulence factor, HylB, shows higher activity in strains isolated from cases of preterm birth than those isolates from rectovaginal swabs of healthy women. We discovered that GBS rely on HylB to avoid immune detection in uterine tissue, but not placental tissue, which leads to increased rates of fetal injury and preterm birth. These studies provide novel insight into the underlying mechanisms of ascending infection.

Infections in pregnancy

2010 ◽  
pp. 2165-2172
Author(s):  
Lawrence Impey
Keyword(s):  
Perinatal Death ◽  
Group B Streptococcus ◽  
Treponema Pallidum ◽  
Neonatal Infection ◽  
In Utero ◽  
Carrier Status ◽  
Maternal Illness ◽  
Group B ◽  
Transplacental Infection ◽  
In Pregnancy

Maternal illness is often more severe in pregnancy, e.g. varicella, malaria, and the treatment of infections in pregnancy is complicated by potential effects of drugs on the fetus. Peri- and postpartum maternal infection is a major cause of maternal mortality. The effects of infection in pregnancy can be broadly categorized as follows (these are not mutually exclusive): (1) transplacental infection causing fetal malformation, e.g. treponema pallidum, rubella; (2) transplacental infection causing severe in utero illness, e.g. parvovirus; (3) neonatal infection / carrier status as a result of transplacental or intrapartum infection, e.g. HIV, herpes zoster; such neonatal infection may be severe; (4) preterm delivery, late miscarriage, perinatal death and cerebral palsy at term delivery are more common in the presence of in utero and placental infection (chorioamnionitis), e.g. Group B streptococcus....

Fetal effects of maternal infection

2020 ◽  
pp. 2678-2686
Author(s):  
Lawrence Impey
Keyword(s):  
Perinatal Death ◽  
Group B Streptococcus ◽  
Treponema Pallidum ◽  
Neonatal Infection ◽  
In Utero ◽  
Carrier Status ◽  
Maternal Infection ◽  
Group B ◽  
Transplacental Infection ◽  
In Pregnancy

This chapter looks at the fetal effects of maternal infection. Immunity is mildly suppressed in pregnancy, and the fetal immune system is developmentally immature. Infections in pregnancy can therefore be devastating both for the mother, as is occasionally seen with varicella, and for the fetus, as exemplified by congenital infections such as those caused by rubella, cytomegalovirus, syphilis, and toxoplasmosis. The fetal effects of maternal infection in pregnancy can be broadly categorized as follows (these are not mutually exclusive): transplacental infection causing fetal malformation (e.g. treponema pallidum, rubella); transplacental infection causing severe in utero illness (e.g. parvovirus); neonatal infection/carrier status as a result of transplacental or intrapartum infection (e.g. HIV, herpes zoster); such neonatal infection may be severe; preterm delivery, late miscarriage, perinatal death, and cerebral palsy at term delivery are more common in the presence of in utero and placental infection (chorioamnionitis) (e.g. group B streptococcus).

scholarly journals Lack of diagnostic-escape mutants of group B streptococcus in Slovenia

2021 ◽  
Author(s):  
Tina Perme ◽  
Daniel Golparian ◽  
Magnus Unemo ◽  
Samo Jeverica
Keyword(s):  
Group B Streptococcus ◽  
Escape Mutants ◽  
Group B
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