Table 3.
Physiologic and clinical effects of obesity on labor
| Effect of obesity on labor physiology | Clinical observation | Possible physiologic mechanism |
|---|---|---|
| Disruption of endocrine signaling initiating labor onset | Delayed onset of parturition | Decreased CRH leading to inhibited functional progesterone withdrawal[55] |
| Decreased cervical ripening | Elevated leptin disrupts collagen degradation and cervical cell apoptosis[61, 62] | |
| Decreased spontaneous rupture of membranes | Elevated leptin inhibits membrane apoptosis[61, 62] | |
| Disruption of uterine contractility | Inadequate uterine contractions leading to increased risk for active phase cesarean | Elevated leptin, visfatin, and apelin inhibit spontaneous and oxytocin augmented uterine contractility in rats in vitro[43, 61, 62] |
| Cholesterol inhibits spontaneous and oxytocin augmented uterine contractility in vitro[65, 66] | ||
| Hypercholesterolemia activates potassium channels and may have effects on estrogen receptors and oxytocin receptors[139, 140] | ||
| Increased required oxytocin doses | Mechanism is unknown, however BMI is not associated with oxytocin receptor gene expres- sion[141, 142] | |
| Disruption of contraction synchronization | Irregular uterine contractions or decreased intrauterine pressure | Uterine biopsies show decreasing connexin-43 (gap junctions) mRNA in dystocia compared to normal labor[136] |
| Rats with high cholesterol diet showed lower con- nexin-43 expression although contractility was not examined[66, 143] | ||
| Metabolic fatigue | Inadequate uterine contractions with poor response to oxytocin augmentation | Increased BMI is associated with excess placental ROS and decreased ATP production[58, 63, 64] |
CRH corticotropin releasing hormone, BMI body mass index, mRNA messenger RNA, ATP adenosine triphosphate