Maternal-Fetal Relations Clinical Trial
Official title:
Determinants of Fetal Inflammatory Exposure at Term
The hypothesis of this study is that maternal and fetal biologic variation in the balance
between pro-inflammatory and anti-inflammatory mediators can be measured by currently
available techniques. In addition, the investigators hypothesize that a pro-inflammatory
maternal phenotype increases the risk of fetal exposure to intrauterine hyperthemia and
inflammatory cytokines; and that intrapartum events, especially known risk factors for fever
at term such as epidural analgesia and prolonged rupture of membranes, may interact with
underlying maternal factors to increase fetal exposure to inflammatory cytokines.
This experiment aims to establish the first large-scale cohort to evaluate biomarkers for
maternal and fetal inflammation in term pregnancy and to elucidate the relative antepartum
and intrapartum contributions to fetal inflammation.
It has been demonstrated that intrapartum fever >100.4 degrees Fahrenheit is associated with
increased maternal and fetal levels of interleukin-6 (IL-6) at delivery. Maternal and fetal
IL-6 levels are highly correlated, and placental transport of cytokines has been
demonstrated. While intrapartum fever is traditionally attributed to acquired infection
(chorioamnionitis), our data indicate that the maternal inflammatory balance assessed prior
to the onset of labor may be a significant determinant of subsequent intrapartum fever. The
increased risk of neonatal brain injury may be cytokine mediated or may, in part, be
secondary to increased vulnerability to hypoxic injury in the setting of elevated fetal
brain temperature.
The baseline prevalence of intrapartum fever at term is 1-5%. Factors associated with an
increased risk of intrapartum fever include maternal age, nulliparity (75%), Hispanic race,
induction and longer labor. However, in recent years, the most potent risk factor for
intrapartum fever has clearly been epidural analgesia - which is selected for intrapartum
pain relief by the majority of mothers in the US especially in the first, most painful
birth. We have demonstrated that the risk of fever after epidural analgesia increases with
increasing duration of epidural analgesia - therefore, the risk of fever after epidural
analgesia is largely confined to nulliparous women. Multiparous women deliver shortly after
the onset of active labor, resulting in a short duration of exposure to epidural analgesia,
and are not at increased risk. Randomized studies demonstrate that the independent
contribution of epidural analgesia to intrapartum fever risk is 3 to 7-fold. Rates of
intrapartum fever >100.4 degrees Fahrenheit in nulliparas with epidural analgesia range from
14.5% to 33%. Rates at the upper end of this range are observed in large, public hospitals
with primarily Hispanic populations. Conversely, lower rates are observed at private
hospitals with primarily Caucasian populations.
This study will make observations based upon:
1. 10 mL of blood drawn the day of enrollment
2. 10 mL of blood drawn upon admission to Labor and Delivery
3. A sample of spinal fluid if a spinal epidural is chosen by the patient
4. Blood collected from the placenta and umbilical cord
In addition, the mother's temperature will be taken every hour during labor.
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Observational Model: Cohort, Time Perspective: Prospective
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